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Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products (2002)

Chapter: Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop

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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Biomedical Applications of Marine Natural Products: Overview of the 2001 Workshop

INTRODUCTION

Marine biotechnology has demonstrated its potential across a broad spectrum of applications that range from biomedicine to the environment. Nevertheless, despite noteworthy successes (Tables 13) and the inherent promise of the ocean’s vast biological and chemical diversity, marine biotechnology has not yet matured into an economically significant field. Fundamental knowledge is lacking in areas that are pivotal to the commercialization of biomedical products and to the commercial application of biotechnology to solve marine environmental problems, such as pollution, ecosystem disease, and harmful algal blooms.

To identify hurdles that are slowing the implementation of marine biotechnology within the biomedical and environmental sciences, the Ocean Studies Board (OSB) and the Board on Life Sciences (BLS) of the National Research Council (NRC) convened two workshops on marine biotechnology. One examined issues limiting the application of biotechnology to marine environmental science (October 1999; National Research Council, 2000), and the other examined issues surrounding biomedical benefits from marine natural products (November 2001).

In this report, the OSB and BLS ad hoc Committee on Marine Biotechnology summarize and integrate information obtained from the two workshops and highlight areas where new investments are likely to pay the

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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highest dividends in fostering the implementation of marine biotechnology in the environmental and biomedical arenas.

DRUG DISCOVERY AND DEVELOPMENT

The U.S. public is aware of the societal benefit of effective drug therapy to treat human diseases and expects that treatment will improve and become ever more accessible to the nation’s population. This expectation is predicated on a continued and determined effort by academic scientists, government researchers, and private industry to discover new and improved drug therapies. Natural products have had a crucial role in identifying novel chemical entities with useful drug properties (Newman et al., 2000). The marine environment, with its enormous wealth of biological and chemical diversity (Fuhrman et al., 1995; Field et al., 1997; Rossbach and Kniewald, 1997), represents a treasure trove of useful materials awaiting discovery. Indeed, a number of clinically useful drugs, investigational drug candidates, and pharmacological tools have already resulted from marine-product discovery programs (Table 1). However, a number of key areas for future investigation are anticipated to increase the application and yield of useful marine bioproducts (see Fenical, p. 45 in this report). The broad areas where advances could have substantial impact on drug discovery and development are (1) accessing new sources of marine bioproducts, (2) meeting the supply needs of the drug discovery and development process, (3) improving paradigms for the screening and discovery of useful marine bioproducts, (4) expanding knowledge of the biological mechanisms of action of marine bioproducts and toxins, and (5) streamlining the regulatory process associated with marine bioproduct development.

New Bioproduct Discovery and Supply

The ocean is a rich source of biological and chemical diversity. It covers more than 70% of the earth’s surface and contains more than 300,000 described species of plants and animals. A relatively small number of marine plants, animals, and microbes have already yielded more than 12,000 novel chemicals (Faulkner, 2001).

Unexamined habitats must be explored to discover new species. Most of the environments explored for organisms with novel chemicals have been accessible by SCUBA (i.e., to 40 meters). Although some novel chemicals have been identified at high latitudes, such as the fjords of British Colum-

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

TABLE 1 Some Examples of Commercially Available Marine Bioproducts

Product

Application

Original Source

Pharmaceuticals

Ara-A (acyclovir)

Antiviral drug (herpes infections)

Marine sponge, Cryptotethya cryta

Ara-C (cytosar-U, cytarabine)

Anticancer drug (leukemia and non-Hodgkin’s lymphoma)

Marine sponge, Cryptotethya cryta

Molecular Probes

Okadaic acid

Phosphatase inhibitor

Dinoflagellate

Manoalide

Phospholipase A2 inhibitor

Marine sponge, Luffariella variabilis

Aequorin

Bioluminescent calcium indicator

Bioluminescent jellyfish, Aequora victoria

Green fluorescent protein (GFP)

Reporter gene

Bioluminescent jellyfish, Aequora victoria

Enzymes

Vent and Deep Vent DNA polymerase (New England BioLabs)

Polymerase chain reaction enzyme

Deep-sea hydrothermal vent bacterium

Nutritional Supplements

Formulaid (Martek Biosciences)

Fatty acids used as additive in infant formula nutritional supplement

Marine microalga

Pigment

Phycoerythrin

Conjugated antibodies used in ELISAs and flow cytometry

Red algae

Cosmetic additives

Resilience (Estée Lauder)

“Marine extract” additive

Caribbean gorgonian, Pseudopterogorgia elisabethae

 

SOURCE: Adapted from Pomponi (1999).

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

bia and under the Antarctic ice, the primary focus of marine biodiversity prospecting has been the tropics. Tropical seas are well-known to be areas of high biological diversity and, therefore, logical sites of high chemical diversity. Much of the deep sea is yet to be explored, and very little exploration has occurred at higher latitudes. With rare exceptions (e.g., the analysis of deep-sea cores to identify unusual microbes), marine organisms from the deep-sea floor, mid-water habitats, and high-latitude marine environments and most of the sea surface itself have not been studied. The reason for this deficiency is primarily financial: oceanographic expeditions are expensive, and neither federal nor pharmaceutical-industry funding has been available to support oceanographic exploration and discovery of novel marine resources. The potential for discovery of novel bioproducts from yet-to-be discovered species of marine macroorganisms and microorganisms (including symbionts) is high (see Carter, p. 47 in this report; de Vries and Beart, 1995; Cragg and Newman, 2000; Mayer and Lehmann, 2001).

To optimize identification of marine resources with medicinal potential, the best tools for discovery must be used at all stages of exploration: in new locations, for collection of organisms never before sampled, and for the identification of chemicals with pharmaceutical potential. Increased sophistication in the tools available to explore the deep sea has expanded the habitats that can be sampled and has greatly improved the opportunities for discovery of new species and the chemical compounds that they produce. New and improved vehicles are being developed to take us farther and deeper in the ocean. These platforms need to be equipped with even more sophisticated and sensitive instruments to identify an organism as new, to assess its potential for novel chemical constituents, and if possible, to nondestructively remove a sample of the organism. Tools and sensors that have been developed for space exploration and diagnostic medicine need to be applied to the discovery of new marine resources.

Perhaps the greatest untapped source of novel bioproducts is marine microorganisms (see Fenical, p. 45 in this report; Bentley, 1997; Gerwick and Sitachitta, 2000; Gerwick et al., 2001). Although new technologies are rapidly expanding our knowledge of the microbial world, research to date suggests that less than 1% of the total marine microbial species diversity can be cultured with commonly used methods (see Giovannoni, p. 65 in this report). That means chemicals produced by as many as 99 percent of the microorganisms in the ocean have not yet been studied for potential commercial applications. These organisms constitute an enormous un-

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

tapped resource and opportunity for discovery of new bioproducts with applications in medicine, industry, and agriculture. Developing creative solutions for the identification, culture, and analysis of uncultured marine microorganisms is a critical need.

With the enormous potential for discovery, development, and marketing of novel marine bioproducts comes the obligation to develop methods for supplying these products without disrupting the ecosystem or depleting the resource. Supply is a major limitation in the development of marine bioproducts (Cragg et al., 1993; Clark, 1996; Turner, 1996; Cragg, 1998). In general, the natural abundance of the source organisms will not support development based on wild harvest. Unless there is a feasible alternative to harvesting, promising bioproducts will remain undeveloped. Some options for sustainable use of marine resources are chemical synthesis, aquaculture of the source organism, cell culture of the macroorganism or microorganism source, and molecular cloning and biosynthesis in a surrogate organism. Each of these options has advantages and limitations; not all methods will be applicable to supply every marine bioproduct, and most of the methods are still in development. Understanding the fundamental biochemical pathways by which bioproducts are synthesized is key to most of these techniques.

Molecular approaches offer particularly promising alternatives not only to the supply of known natural products (e.g., through the identification, isolation, cloning, and heterologous expression of genes involved in the production of the chemicals) but also to the discovery of novel sources of molecular diversity (e.g., through the identification of genes and biosynthetic pathways from uncultured microorganisms) (Bull et al., 2000). Manipulation of heterologously expressed secondary metabolite biosynthetic genes to produce novel compounds having potential pharmaceutical utility is at the forefront of current scientific achievements and has tremendous potential for creation of novel chemical entities (see Moore, p. 61 in this report; Khosla et al., 1999; Du and Shen, 2001; Floss, 2001; Rohlin et al., 2001; Staunton and Wilkinson, 2001; Xue and Sherman, 2001). In approaches parallel to those used for terrestrial soils, efforts need to be made to clone useful secondary metabolite biosynthetic pathways from natural assemblages of marine microorganisms (e.g., “cloning of the ocean’s metagenome”). Use of these approaches to provide solutions to natural-product supply and resupply problems should be increased.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Screening for Bioactivity

Screening of natural materials for biologically active compounds has undergone radical changes over the past decade. With the advent of high-throughput-screening (HTS) technologies, an enormous number of materials, over 600,000, can be screened for a particular biological or biochemical property in a relatively short time, 2 to 4 months (Landro et al., 2000; Engels and Venkatarangan, 2001; Manly et al., 2001). Hence, a screen for a given disease target may be in operation for 3 months, during which time, marine natural products will be competing with large libraries of synthetic chemicals. New strategies for handling natural-product “mixtures” must be developed to synchronize with the accelerated HTS timetables. Marine natural-product mixtures, or extracts, must be purified and their active components rapidly identified. Development of technology to allow the prefractionation of crude extract materials prior to biological assay may allow for the rapid examination of active compound structures.

Another arena for improvement is the efficient elucidation of known and new natural-product structures. Hybrid analytical techniques that combine high-performance liquid chromatography (HPLC) with mass spectrometry (MS) and nuclear magnetic resonance (NMR) spectroscopy are becoming more common and accessible to natural-products chemists, and use of such techniques will expand in a variety of scholarly settings (Peng, 2000; Wilson, 2000). Continuous technological advances are needed in analytical chemistry associated with marine drug discovery to keep pace with comparable advances in biological screening of natural materials.

Currently, investigators do not have access to a broad range of biological assays for marine bioproduct discovery. Innovative strategies are needed that link groups of investigators to efficient drug-discovery programs. Such partnerships are envisioned for broad evaluations of new marine biomaterials in assays targeting a more complete range of human diseases (e.g., infectious, cardiovascular, cancer, neurodegenerative diseases, allergy and inflammation, and other metabolic disorders) as well as agricultural and veterinary needs. The increased number of discoveries of biomaterials possible through these partnerships and a corresponding improvement in the sophistication of their handling and distribution will encourage greater industrial evaluation of novel marine bioproducts.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Understanding Mechanisms of Action

The clinical and commercial development of many marine natural products languishes because of insufficient knowledge of how the compounds function in biological systems (Faulkner, 2000). It is precisely this understanding of pharmacological mechanism of action that has driven the development of such well-known pharmaceuticals as the potent anticancer metabolite paclitaxol (Taxol) from the Pacific yew tree (see Jordan and Wilson, p. 52 in this report; Correia and Lobert, 2001). Strategies that might be used in accelerating the development of marine biomaterials include focused mechanism-of-action studies, screening of libraries of purified marine metabolites by mechanism-based high-throughput assays, and characterization of a compound’s biological effect using functional genomic and proteomic approaches. At the same time, it is crucial to make advances in integrated pharmacology to understand the effects of new and experimental drug therapies at the molecular, cellular, organ, and whole-animal levels. Molecularly based chemical ecological studies are a complementary approach to learn how marine biomaterials exert their properties in nature. In general, a greater emphasis on studying the mechanisms by which marine metabolites exert their potentially valuable properties will translate into an increased number of clinical candidates entering the development pipeline.

Marine organisms have demonstrated their utility as models to understand disease processes in humans (Table 1) (see Walsh, p. 57 in this report). Priority should be given to the identification and development of new model marine organisms to (1) identify novel targets for disease therapy, (2) discover novel chemicals for drug development, and (3) provide alternatives to current animal (and human) testing of drugs. With more complete genome sequences available from novel organisms, it will be more likely that an analog to human mutations can be found in a convenient test organism. Of critical importance in the development of new models is the availability of genome sequences from marine organisms. Genomic approaches, including whole-genome studies of appropriate model organisms, will accelerate discovery of new targets and new marine-derived drugs.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Recommendations for Enhancing Drug Discovery with Marine Biotechnology

  • Explore new habitats.

  • Develop tools to discover new resources.

  • Discover and culture new marine microorganisms (including symbionts).

  • Provide sufficient supply of bioproducts.

  • Develop new screening strategies.

  • Pursue strategies to hasten the discovery of new materials.

  • Combine resources of academic, governmental, and industrial laboratories to expand access to biological screens in a variety of therapeutic areas.

  • Expand research on pharmacological mechanisms.

  • Establish new marine model organisms.

  • Expand research on marine bioproduct biosynthesis and molecular biology.

GENOMICS AND PROTEOMICS APPLICATIONS FOR MARINE BIOTECHNOLOGY

Genomics

Genomics is the sequencing, annotating, and interpreting of information contained within the genome of an organism. Genome sequences of microorganisms represent the majority of the earliest work in genomics (Fraser et al., 2000a,b; Nelson et al., 2000) and have led to a better understanding of the biology of the organisms sequenced (Nierman et al., 2000). Microorganisms have been the focus of genomic research, probably because they have smaller genomes and therefore represent a more manageable sequencing goal. Recent technological breakthroughs in automated DNA sequencing and computational power have made it possible to rapidly sequence and annotate even large or complex genomes (Nelson et al., 1999; Heidelberg et al., 2000). Representations of the entire metabolic potential of microorganisms derived from the application of bioinformatics have indicated the presence of hitherto unsuspected metabolic pathways in even some very-well-characterized bacteria. Such genomic information provides a new basis for understanding physiological processes, such as responses of indicator species to environmental changes, stimuli that cause

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

an organism to synthesize a product of potential human benefit, or discovery of new gene targets for drug therapy, to name just a few (Read et al., 2001). The pharmaceutical industry has taken advantage of microbial genomics to search for novel vaccine targets in pathogenic microorganisms, greatly reducing the time and cost of drug target discovery (Pizza et al., 2000).

We have learned a tremendous amount during the infancy of the “genomic revolution.” During this early period of genomic research, both basic and applied scientific questions have been addressed, and many have been answered. The ability to determine fully the genomic structure of an organism has allowed for finer resolution and greater speed in addressing specific biomedical questions, such as determining potential vaccine candidates from bacterial pathogens (Saunders et al., 2000). The genomic revolution has also led to the discovery of novel processes with major ecological implications, such as a rhodopsin-driven proton pump in an abundant but uncultured proteobacterium from the ocean’s surface. This discovery— based on the application of genomics to analyses of easily collected but uncultured marine microorganisms—has opened a new path to understanding of light-harvesting and near-surface open-ocean primary productivity (Béjà et al., 2000, 2001).

Current genomic methods enable researchers greater speed, sensitivity, and resolution over other commonly used molecular methods. As the science of genomics continues to mature, new technologies will emerge. Their implementation and integration with other technologies will be essential for advancement in the marine biomedical and environmental sciences (Cary and Chisholm, 2000).

With recent decreases in sequencing costs and increases in the number of high throughput sequencing facilities at private, governmental, and nonprofit laboratories in the United States, complete genome sequencing of many established and novel model organisms, including eukaryotic marine organisms, is realistically attainable (Fraser, p. 66 in this report). In addition, the development of genomic technologies, such as bacterial artificial chromosomes (BACs) enabling the cloning of large DNA fragments, and the expansion of computational tools for genomic analysis now allow the complete sequencing and genomic analysis of entire biological systems to be an achievable goal. Many marine eukaryotic organisms (e.g., corals, sponges, and tube worms) maintain large and diverse populations of microbial symbionts. The complete genome sequences of these consortia will not only lead to unprecedented understanding of the interactions be-

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

tween host and symbiont, but will also expedite the discovery of novel metabolites, such as drugs and fine chemicals, that are the products of such consortia.

As much as 40% of a genome encodes for genes whose functions remain unknown, highlighting genome sequencing and annotation as a parts list, but not the organism’s instruction manual. These unknown gene functions represent a starting point for scientists studying either a specific organism or a biological relationship (e.g., host and symbiont). However, for complete genome sequences to be utilized by the greatest number of scientists possible, particular species or strains must be identified and carefully selected as models (see Walsh, p. 57 in this report). Genomic information should enable as large a scientific community as possible to expand its current research; the selection of an inappropriate organism will not allow for a broad application. Although the cost of sequencing has decreased, it is still important not to waste effort on redundant genomic projects. To reduce duplication of effort, the sequence data and the databases and tools that allow scientists to analyze and utilize the data must be maintained and made accessible. Additionally, projects that require sequencing of large genomes must be subjected to a careful cost and value analysis of finished genome versus draft sequencing (a less expensive approach, with missing genes and misassembled regions of the genome). The scientific community at large must take responsibility for many of these pragmatic considerations, selection of appropriate model species for sequencing, maintenance of publicly accessible databases, and determination of the relative value of finished genome versus draft sequencing.

Marine Microbes and Genomics

A large and interesting pool of potentially bioactive molecules is likely to be affiliated with the microbial population of the oceans (see Fenical, p. 45, and Giovannoni, p. 65 in this report). These populations are typically composed of a few cosmopolitan organisms, but the overall group diversity is very high. It has been a problem to bring many of these organisms into culture where they can be studied more easily. Currently, methods are being developed that have allowed several of these cosmopolitan marine bacteria to be cultured.

There are numerous other marine microorganisms that have not been cultured. Some of these bacteria might be culturable when more innovative approaches are developed (see Giovannoni, p. 65 in this report). How-

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

ever, it is unlikely the species diversity of the oceans will be brought completely into pure culture. As a more tractable alternative, genomic and bioinformatic methods are powerful new tools to access the gene products of these uncultured microorganisms. The total DNA from an environmental sample can be purified without first culturing the organisms (Ward et al., 1990, 1992; Rondon et al., 2000). This environmental DNA can be sequenced analogously to a genome and allows access not only to the protein products of uncultured bacterial species, but also to the genomic potential of the environment (or “ecological genomics”). The current technology is already in place for such survey sequencing of environmental DNA. Following bioinformatic analysis, cloning and expression of selected genes from the uncultured bacteria will likely lead to the discovery of novel bioactive molecules. These methods have been used successfully in looking for antimicrobial proteins from uncultured soil bacteria.

DNA Microarrays

Microarray technologies offer an additional tool for high-throughput analyses of the genome of an organism and the responses of an organism to specific changes. In an organismal DNA microarray, thousands of protein-encoding DNA sections are arrayed on a solid support structure (e.g., glass slide or nylon membrane). The array is then hybridized with a nucleic acid from a test sample, and the genes common to both the microarray and the test sample can be detected. As one example of an application of DNA microarray technology, the nucleic acid test sample can be the total messenger RNA (representing those genes that are likely being expressed as proteins) isolated before and after introduction of an environmental stress (e.g., addition of a pollutant, challenge with a bioactive molecule, and change in temperature). In this case, the genes that the organism differentially expresses as a result of the stress can be determined. Therefore, microarrays can be useful tools to examine gene expression patterns of a model organism in response to a variety of stimuli. That capability makes them powerful new diagnostic tools with applications in environmental monitoring, bioremediation, and drug discovery and reiterates the importance of careful selection by the scientific community of model organisms for complete genome sequencing. Obviously, this tool is most powerful for organisms for which the complete genome is sequenced, but even if expressed sequence tags (ESTs) are spotted on the microarray, experiments can yield very useful information (see Walsh, p. 57 in this report).

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Microarray techniques also are powerful tools for examining the genomic differences between two organisms, particularly if a complete reference genome is available for comparisons. The total genomic DNA of the second organism is used as the test sample for hybridization to the genome microarray of the first organism. These data allow rapid determination of the genes found on the reference genome and genes shared between the two organisms. Such comparisons to reference genomes are very useful to identify genes that are distinctive to different individuals or strains from different environments. Medical microbiologists have taken advantage of such comparisons to find pathogenicity “islands” in disease-causing bacteria. By sequencing and building a genome array of a pathogenic bacterial strain and hybridizing the array with less pathogenic strains of the same species, genomic regions resulting in increased pathogenicity have been determined (see Fraser, p. 66 in this report). Analogously, the genes responsible for the production of bioactive molecules by marine eukaryotes or prokaryotes can be more quickly determined after the genome sequence of the model organism is determined and a complete genome array constructed.

As microarray methods become more common, duplication of effort and resources is more likely. Much of the cost of microarray technology is in the design and production of the test slide. If care is not taken, individual researchers might waste important time and effort producing duplicate microarrays for the same species. One way to reduce the risk of duplication is through centralization of a microarray production facility, either virtual or physical, for community-wide use. Such a facility may also help to standardize methods and allow comparisons of experiments conducted in different laboratories.

Proteomics

Proteomics is the characterization of the proteins specified by the genome of an organism. Proteomics is a new science that is considered to be an extension of the Human Genome Project, because it links genetics with physiology and provides clues not only to the function of genes encoding certain proteins but also to the function of the proteins. There are molecular techniques that allow determination of expressed proteins in a given system. However, these techniques are very time-consuming when used to identify the posttranslational modification of proteins. An understanding of the modification of proteins will become increasingly more important in the search for novel biomolecules.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

The potent combination of classic microbiological techniques, proteomics, and genomics must be recognized. Lab culture of microorganisms, when linked with genomic analysis and the use of proteomics, represents a continuum of knowledge about the adaptations of microbes to their changing environments. Intersections of these three investigative paths may provide crucial information for identifying novel metabolites, pathogens, and for characterizing environmental remediation needs.

Unfortunately, proteomic methods are not yet high throughput and are fairly costly when considering analyses of an entire genome. As these technologies develop, especially at the national laboratories, it will be important for proteomics to be integrated into marine biomedical and environmental research programs.

Genomics and Proteomics as Exploration Science

Genomic studies are not always hypothesis driven; their fields are exploratory. The technology enables scientists to generate data from which hypotheses can be formulated and tested. This exploration activity should be considered an asset because of its potential to increase our knowledge base, and it should not be considered a liability, particularly in the review of proposals incorporating genomics and proteomics technologies. It is important to make certain, however, that genomic and proteomic data are publicly available, and in a useful form so that the data can be used for hypothesis-driven research. Therefore, it is important that genomic and proteomic databases be developed, maintained, and made available as research tools.

Recommendations to Enhance the Application of Genomics and Proteomics to Marine Biotechnology

  • Incorporate genome sequencing, proteomics, and bioinformatics with nonculture-based methods to survey diverse marine environments and improve screening methods for uncultured microbes.

  • Ensure that high-throughput sequencing and informatics facilities are available to the marine biotechnology research community.

  • Develop a community-wide consensus on model organisms for genome sequencing, and develop both a priority list and a “wish” list.

  • Develop arrays for determining differences among the genomes of different organisms.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×
  • Develop whole-genome and EST arrays to determine gene-expression patterns of model organisms as rapid screens for bioactivity and drug discovery.

  • Develop environmental genome microarray chips to identify function or coregulation of genes from the environment.

  • Determine the potential usefulness of a centralized microarray facility to make reagents, develop and disseminate informatics tools, and provide training to the marine biotechnology community. Reduce redundant funding of array development and nonstandardized hybridization techniques that will prevent cross-experiment comparisons.

  • Ensure that the “exploratory” data generated in both genome sequencing and functional genomic studies are available to expedite and enable hypothesis-driven science. Include the development and maintenance of useful public databases and improved training of the scientific community.

BIOMATERIALS AND BIOENGINEERING

Well beyond the obvious providers of food, the world’s seas have always been bountiful providers of special materials valued for human health and pleasure. Access to this resource historically has been hindered by the apparent hostility of the seawater environment to manufactured materials and engineering concepts of terra firma. In spite of the extraordinary potential of the marine environment for new biomaterials, the environmental risks and exploration costs have been prohibitive.

In the past decade, new tools of biotechnology have been introduced that are producing extraordinary new products and assays based on the new understanding of genetic factors and their expression as complex biological molecules. Applying these tools to the marine environment provides opportunities to unlock similar micro-molecular vaults of marine biomedical products so that they can join other macro-biomaterials already harvested from the sea for thousands of years.

Novel Characteristics of Macro-Biomaterials from Marine Organisms

Marine biomaterials are a heterogeneous group of organic-, ceramic-, and polysaccharide-based polymers that hold promise for a variety of new approaches to the treatment of disease (see White and White, p. 79, and Laurencin, p. 83 in this report). The marine environment is home to

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

numerous microporous materials, such as those that provide the framework for coral reefs or those that compose the spines of sea urchins. These macro-biomaterials are characterized by highly interconnected porous networks, with a wide range of porosities (Weber and White, 1973). Because of their geometric and material properties, coral structures and urchin spines are used in vascular graft construction and orthopedic surgical repairs (see White and White, p. 79 in this report). Identification of the natural convoluted geometries and fouling-resistant surface features of coral has been a key factor prompting consideration of other biotechnology approaches to successful biomimicry and biomaterials manufacture. Marine organisms can provide many more novel models for biomolecular materials design.

New biotechnologies have been introduced for biocompatible, self-limiting, implantable biomedical devices based on “storage biopolymers,” such as polyhydroxyalkanoates, which are abundant in marine microorganisms (see Laurencin, p. 83 in this report; Madison and Huisman, 1999). New opportunities also exist for high-value biomedical products, such as drug-delivery units, based on chitin from marine crabs and other crustaceans (Felt et al., 1998; Janes and Alonso, 2001; Sato et al., 2001). The enormous supply of chitin and chitosan biopolymers serves as a base for hydrogel-like hosts for various medicinal ingredients, including antibiotics, and provides good wound-dressing qualities for abrasions and ulcers. Work is under way to utilize novel combinations of storage biopolymers, particularly polyhydroxybutyrate, with coral segments to fabricate a scaffold that can be used in bone repair (Laurencin et al., 1996; Madihally and Matthew, 1999; Suh and Matthew, 2000).

Facilitating Work at Surfaces

Marine surfaces are important planes of research and exploration for biotechnological applications. Of particular interest are the characteristics of submerged natural surfaces that resist corrosion and adhesion and the opposing characteristics of selected organisms that allow them to adhere tightly to wet, slimy surfaces. The oceans’ intrinsically nonstick, low-drag plant and animal surfaces and the adaptations of some species to adhere to wet surfaces hold incredible promise for future biomedical applications (Anderson, 1996). The most well-known example is perhaps the common blue mussel, Mytilus edulis, with its strong byssal threads, and adhesion discs which allow it to remain attached in very high energy environments, including pounding surf. However, to fully commercialize these character-

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

istics, critical issues of cross link biocatalysis and water displacing post-translational modifications of secreted adhesive biopolymers must be resolved (see Benedict, p. 69 in this report). In addition to the submerged biological and physical surfaces, the air-sea interface is important as a biomaterial source and model for bioengineering of new artificial lungs and biolubricants. The sea surface is ubiquitously coated with surface-active natural molecules that are the modulators of gas and particle exchange across the liquid-gas interface. Similar analogies exist between sea-surface films and natural biolubricants of human tear films in the blinking human eye.

Applications for Novel Marine Biomaterials

There are many areas in which a better understanding of physiological processes in marine organisms may improve the development of biomedical tools. For example, coral growth and healing may improve the understanding of bone development and healing. A better understanding of the principles of biomimicry of marine surfaces may allow the development of micro- and nano-structured implants for tissue regeneration. Sea-surface explorations should be a routine part of deep sea and coral examinations for materials with bioengineering and tissue-engineering applications. New photocatalytic materials will likely be found in the uppermost sea-surface zones otherwise neglected in explorations of deep sea and coral surfaces, as evidenced by the recent discoveries of light-driven photopigment reactions near the sea-air boundary (Béjà, et al., 2000, 2001).

Biotechnological tools may reveal how marine biocatalysis promotes secure underwater adhesion, with strength and security yet unmatched by terrestrial sources and synthetic approaches. Underwater self-cleaning, self-lubricating plant and animal surfaces may be better understood with new biotechnology, the results of which could be used for the benefit of dry eye and dry mouth sufferers and lubricant-depleted human tissues.

The sustained productivity and economic successes of collection and bioengineering of kelp and other macroalgal products into agars, alginates, and food products provide models for the future of marine biotechnology as it applies to marine biomaterials. Another goal is to identify and exploit the micro- and nano-scale novel characteristics of marine organisms that can make excellent templates for biomaterials and drug delivery of therapeutic devices with potential application in human medicine and bioengineering.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Recommendation for Enhancing Development of Marine Biomaterials

  • Explore for new sources and characterize the novel physical and chemical characteristics of marine biomaterials for potential innovative biomedical and environmental engineering applications including biomolecular materials design.

PUBLIC POLICY, PARTNERSHIPS, AND OUTREACH IN MARINE BIOTECHNOLOGY

Although marine biotechnology has an expanding impact on biomedical, agrichemical, and environmental applications, important knowledge gaps still exist. More discussion among scientists, private businesses, legislators, and the public must be organized to ensure broader implementation and commercialization of products. These gaps include issues of intellectual property rights, mechanisms of technology transfer, knowledge of regulatory requirements (Gerhart, p. 94 in this report), resource sustainability (Bruckner, p. 87 in this report), and the importance of forging partnerships between and among the various constituent stakeholders (see Rosenthal, p. 91, and Cato and Seaman, p. 97 in this report). Businesses, legislators, and the public need to understand the importance and promise of ocean biodiversity as a source for marine biotechnological innovation and recognize the promise and problems of marine biotechnology as they specifically relate to environmental and biomedical applications.

Intellectual Property Rights and Technology Transfer

The commercial development of marine bioproducts is complex, time-consuming, expensive, and risky (see Gerhart, p. 94 in this report). Thus, protection of an individual’s intellectual property rights through patents, copyrights, trade secrets, or trademarks for a potential product is essential for encouraging commercial development of that product (Smith and Parr, 1998). However, academic environments create special challenges for individual patent protection, primarily because academic culture is based on intellectual freedom, open discourse, and individual achievement. The role of the university is viewed as one of creating and disseminating knowledge, not withholding and protecting information. Indeed, most university research is externally funded, and investigators are expected to publish exten-

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

sively. Thus, a fundamental disconnect exists between the general view of the university’s mandate for openness and access and the need for patent protection to ensure that products and ideas developed within an academic setting can be realistically available for the lengthy and expensive process of commercialization.

To facilitate the interaction of industry and academia, most universities now maintain offices that facilitate technology transfer. The concept of university-industry technology transfer is attributed to Vannevar Bush, science advisor to President Franklin Delano Roosevelt. Initially, the idea was driven by concerns about U.S. national security during World War II. In 1980, the Bayh-Dole Act modernized the concept and stimulated the creation of the university technology transfer programs as we know them today. This act mandates that university researchers must disclose inventions made with federal support and requires universities to report inventions to the U.S. government. According to the act, universities may elect to take title to an invention resulting from federally funded research but notes that if they do so, they must diligently pursue patenting and commercialization. Universities typically accomplish technology transfer through licensing (Abramson et al., 1997).

The Regulatory Process

Federal regulations control the development and marketing of bioproducts with human health and safety implications. Preclinical- and clinical-product development related to the regulatory process can take an average of 5 to 7 years and can cost from $15 million to more than $200 million (Cato, 1988; Trenter, 1999), with some reports of costs as high as $800 million (DiMasi, 2001). This cost can be one of the most important hurdles to surmount in the development of a marine-derived bioproduct. Mechanisms to streamline the process and lower the expense must be explored if marine bioproduct development for medical applications is to succeed.

A look at the marine bioproducts available today through the advances of marine biotechnology suggests that numerous products of marine origin have already been successful. Products have been brought to market (Tables 1 and 2), and ideas have been licensed for commercial development (Table 3). Despite these successes, there are concerns that the potential of many marine bioproducts is being compromised because the transition from labo-

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

TABLE 2 Some Commercially Available Marine-Derived Biomedical Research Probes

Source

Probe

Function

Price

Sponge

Manoalide

Phospholipase A2 inhibitor

$120/mg

Calyculin A

Protein phosphatase inhibitor

$105/25 µg

Luffariellolide

Phospholipase A2 inhibitor

$100/mg

12-epi-scalaridial

Phospholipase A2 inhibitor

$136/mg

Latrunculin B

Actin polymerization inhibitor

$90/mg

Mycalolide B

Actin polymerization inhibitor

$212/20 µg

Swinholide A

Actin microfilament disruptor

$100/20 µg

Dinoflagellate

Okadic acid

Protein phosphatase inhibitor

$75/25 µg

Bryozoan

Bryostatin 1

Protein kinase C activator

$88/10 µg

Sea hare

Dolastatin 15

Microtubule assembly inhibitor

$125/mg

 

SOURCE: BioMol [www.biomol.com].

ratory discovery to early commercial development has not been efficient or successful, and regulatory hurdles have not been surmounted. To overcome these bottlenecks it is necessary to educate marine scientists more aggressively about intellectual property rights and regulatory processes. That education should result in increased invention disclosure rates that will preserve nascent patent rights and ensure that more products are available for commercialization. Efforts should also be made to encourage transitional research, thus enhancing the movement of an idea to marketable product.

Sustaining Resources Through Diverse Partnerships

Because the continued successful development of marine biotechnology is intimately connected with ocean biodiversity, it is essential that efforts be made to ensure that biodiversity is protected. Tropical regions with especially rich biological marine ecosystems are often regions of intense poverty (see Bruckner, p. 87 in this report). Short-term, regional financial incentives, which seem to have an immediate impact on the poverty, must be balanced with the long-term sustainability of the resource. Partnerships must be developed to protect marine resources in tropical areas in particular, thus ensuring a positive economic outcome and the long-term protec-

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

TABLE 3 Marine-Derived Antitumor Compounds Licensed for Development

Marine Source

Drug

Organism

Current Status

Sponge

Discodermolide

Discodermia dissoluta

To enter Phase I trials in 2002; licensed to Novartis

Isohomo-halichondrin B

Lissodendoryx sp.

Licensed to PharmaMar S.A.; in advanced preclinical trials

Bengamide

Jaspis sp.

Synthetic derivative licensed to Novartis; in clinical trials

Hemiasterlins A & B

Cymbastella sp.

Derivatives to enter clinical trials in 2002; licensed to Wyeth-Ayerst

Girolline

Pseudaxinyssa cantharella

Licensed to Rhone Poulenc

Bryozoan

Bryostatin 1

Bugula neritina

In Phase I/II clinical trials in U.S./Europe; U.S. National Cancer Institute (NCI) sponsored trials

tion of the resource (see Rosenthal, p. 91 in this report). In all cases, commercial development from natural populations of marine organisms must be sustainable if it is to make economic sense. Sustainability is one of the central challenges in further development of marine biotechnology, and it must be addressed before large-scale marine harvests can begin. Innovative approaches to partnerships between stakeholders can help to support access to marine resources and to ensure their development as sustainable assets. Agreements that include training and education of local populations can be particularly valuable for long-term resource sustainability.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Marine Source

Drug

Organism

Current Status

Sea hare

Dolastatin 10

Dolabella auricularia

Phase I clinical trials in U.S.; NCI sponsored trials

Tunicate

Ecteinascidin 743

Ecteinascidia turbinata

Licensed to PharmaMar S.A.; in Phase III clinical trials in Europe and in U.S.

Aplidine

Aplidium albicans

In Phase II clinical trials; licensed to PharmaMar S.A.

Isogranulatimide

Didemnum granulatum

Licensed to Kinetik, Canada

Gastropod

Kahalalide F

Elysia rubefescens

In Phase I clinical trials; licensed to PharmaMar S.A.

Actinomycete

Thiocoraline

Micromonospora marina

Licensed to PharmaMar S.A.; in advanced preclinical trials

 

SOURCE: Data from David J. Newman, National Cancer Institute, Natural Products Branch, Frederick, Md.

Enhancing Public Awareness and Understanding of Marine Biotechnology

As marine biotechnology rapidly evolves, there is an increasing gap between use of technology and the public’s understanding of that science and its implications. To avoid the public’s misunderstandings that plague agricultural biotechnology (e.g., genetically modified foods), it is essential that scientists partner with the public to provide information that addresses both the promise and possible problems of marine biotechnology. A multitier approach should be developed that connects individuals from science,

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

education, business, and media to address the public’s formal and informal educational needs (Cato and Seaman, p. 97 in this report).

For marine biotechnology, implementation of improved technology transfer, sustainable environmental stewardship, innovative partnerships, and enhanced public education should result in increased production of marine bioproducts and approved marine therapeutics, enhanced revenues from marine bioproducts, and positive impacts on coastal economic development.

Recommendations to Enhance Research and Development, Partnerships, and Outreach for Marine Biotechnology

  • Aggressively educate marine scientists about intellectual property rights and regulatory processes to increase invention disclosure rates and preserve patent rights so that more products will be available for commercialization.

  • Encourage academic rewards for transitional research between academic and industry scientists to facilitate the commercialization of marine bioproducts.

  • Develop innovative approaches to partnerships between stakeholders to support access to ocean resources and to ensure their use as sustainable assets.

  • Educate the public to the promise and problems of marine biotechnology to avoid fears rooted in misunderstanding and misconception.

  • Enhance technology transfer services in universities.

REFERENCES

Abramson, H. N., J. Encarnação, P. P. Reid, and U. Schmoch, Eds. 1997. Technology Transfer Systems in the United States and Germany: Lessons and Perspectives. Part I: Overview and Comparison. National Academy Press, Washington, D.C.

Anderson, J. M. 1996. Biomaterials and medical implant science: present and future perspectives: a summary report. Journal of Biomedical Materials Research 32:143-147.


Béjà, O., L. Aravind, E. V. Koonin, M. T. Suzuki, A. Hadd, L. P. Nguyen, S. B. Jovanovich, C. Gates, R. A. Feldman, and E. F. DeLong. 2000. Bacterial bacteriorhodopsin: evidence for light-driven proton pumping in the sea. Science 289:1902-1906.

Béjà, O., E. N. Spudich, J. L. Spudich, M. Leclerc, and E. F. DeLong. 2001. Proteorhodopsin phototrophy in the ocean. Nature 411:786-789.

Bentley, R. 1997. Microbial secondary metabolites play important roles in medicine; prospects for discovery of new drugs. Perspectives in Biology and Medicine 40:364-394.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Bull, A. T., A. C. Ward, and M. Goodfellow. 2000. Search and discovery strategies for biotechnology: the paradigm shift. Microbiology and Molecular Biology Reviews 64:573-606.

Cary, S. C., and S. W. Chisholm. 2000. Ecological Genomics: The Application of Genomic Sciences to Understanding the Structure and Function of Marine Ecosystems. Report of a Workshop on Marine Microbial Genomics to Develop Recommendations for the National Science Foundation. National Science Foundation, Arlington, Va.

Cato, A. E. 1988. Clinical Trials and Tribulations. Marcel Dekker, Inc., New York.

Clark, A. M. 1996. Natural products as a resource for new drugs. Pharmacological Research 13:1133-1144.

Correia, J. J., and S. Lobert. 2001. Physiochemical aspects of tubulin-interacting antimitotic drugs. Current Pharmaceutical Design 7:1213-1228.

Cragg, G. M. 1998. Paclitaxel (Taxol): a success story with valuable lessons for natural product drug discovery and development. Medical Research Reviews 18:315-331.

Cragg, G. M., S. A. Schepartz, M. Suffness, and M. R. Grever. 1993. The taxol supply crisis. New NCI policies for handling the large-scale production of novel natural product anticancer and anti-HIV agents. Natural Products 56:1657-1668.

Cragg, G. M., and D. J. Newman. 2000. Antineoplastic agents from natural sources: achievements and future directions. Expert Opinion on Investigational Drugs 9:2783-2797.


de Vries, D. J., and P. M. Beart. 1995. Fishing for drugs from the sea: status and strategies. Trends in Pharmacological Science 16(8):275-279.

DiMasi, J. A. 2001. The economics of pharmaceutical innovation: new estimates of drug development costs. Tufts Center for the Study of Drug Development 25th Anniversary Forum, Four Seasons Hotel, Philadelphia, Pa., November 30, 2001.

Du, L., and B. Shen. 2001. Biosynthesis of hybrid peptide-polyketide natural products. Current Opinions in Drug Discovery and Development 4:215-228.


Engels, M. F., and P. Venkatarangan. 2001. Smart screening: approaches to efficient HTS. Current Opinions in Drug Discovery and Development 4:275-283.


Faulkner, D. J. 2000. Marine pharmacology. Antonie Van Leeuwenhoek 77:135-145.

Faulkner, D. J. 2001. Marine natural products. Natural Product Reports 18:1-49.

Felt, O., P. Buri, and R. Gurny. 1998. Chitosan: A unique polysaccharide for drug delivery. Drug Development and Industrial Pharmacy 24:979-993.

Field, K. G., D. Gordon, T. Wright, M. Rappe, E. Urback, K. Vergin, and S. J. Giovannoni. 1997. Diversity and depth-specific distribution of SAR11 cluster rRNA genes from marine planktonic bacteria. Applied and Environmental Microbiology 63:63-70.

Floss, H. G. 2001. Antibiotic biosynthesis: from natural to unnatural compounds. Journal of Industrial Microbiol Biotechnology 27:183-194.

Fraser, C. M., J. Eisen, R. D. Fleischmann, K. A. Ketchum, and S. Peterson. 2000a. Comparative genomics and understanding of microbial biology. Emerging Infectious Diseases 6:505-512.

Fraser, C. M., J. A. Eisen, and S. L. Salzberg. 2000b. Microbial genome sequencing. Nature 406:799-803.

Fuhrman, J. A., K. McCallum, and A. A. Davis. 1995. Phylogenetic diversity of subsurface marine microbial communities from the Atlantic and Pacific oceans. Applied and Environmental Microbiology 61:4517.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Gerwick, W. H., L. T. Tan, and N. Sitachitta. 2001. Nitrogen-containing metabolites from marine cyanobacteria. P. 75-184 in The Alkaloids, G. Cordell (Ed.), Academic Press, San Diego.

Gerwick, W. H., and N. Sitachitta. 2000. Nitrogen-containing metabolites from marine bacteria. P. 239-285 in The Alkaloids, G. Cordell (Ed.), Academic Press, San Diego.


Heidelberg, J. F., J. A. Eisen, W. C. Nelson, R. A. Clayton, M. L. Gwinn, R. J. Dodson, D. H. Haft, E. K. Hickey, J. D. Peterson, L. Umayam, S. R. Gill, K. E. Nelson, T. D. Read, H. Tettelin, D. Richardson, M. D. Ermolaeva, J. Vamathevan, S. Bass, H. Qin, I. Dragoi, P. Sellers, L. McDonald, T. Utterback, R. D. Fleishmann, W. C. Nierman, O. White, et al. 2000. DNA sequence of both chromosomes of the cholera pathogen Vibrio cholerae. Nature 406:477-483.


Janes, K. A., P. Calvo, and M. J. Alonso. 2001. Polysaccharide colloidal particles as delivery systems for macromolecules. Advanced Drug Delivery Reviews 47:83-97.


Khosla, C., R. S. Gokhale, J. R. Jacobsen, and D. E. Cane. 1999. Tolerance and specificity of polyketide synthases. Annual Review of Biochemistry 68:219-253.


Landro, J. A., I. C. Taylor, W. G. Stirtan, D. G. Osterman, J. Kristie, E. J. Hunnicutt, P. M. Rae, and P. M. Sweetnam. 2000. HTS in the new millennium: the role of pharmacology and flexibility . Journal of Pharmacological and Toxicological Methods 44:273-289.

Laurencin, C. T., M. A. Attawia, H. E. Elgendy, and K. M. Herbert. 1996. Tissue engineered bone-regeneration using degradable polymers: The formation of mineralized matrices. Bone 19:93S-99S.


Madihally, S. V., and H. W. Matthew. 1999. Porous chitosan scaffolds for tissue engineering. Biomaterials 20:1133-1142.

Madison, L. L., and G. W. Huisman. 1999. Metabolic engineering of Poly(3-Hydroxyalkanoates): from DNA to plastic. Microbiology and Molecular Biology Reviews 63:21-53.

Manly, C. J., S. Louise-May, and J. D. Hammer. 2001. The impact of informatics and computational chemistry on synthesis and screening. Drug Discovery Today 6:1101-1110.

Mayer, A., and V. K. Lehmann. 2001. Marine pharmacology in 1999: antitumor and cytotoxic compounds. Anticancer Research 21:2489-2500.


National Research Council. 2000. Opportunities for Environmental Applications of Marine Biotechnology. National Academy Press. Washington, D.C.

Nelson, K. E., R. A. Clayton, S. R. Gill, M. L. Gwinn, R. J. Dodson, D. H. Haft, E. K. Hickey, J. D. Peterson, W. C. Nelson, K. A. Ketchum, L. McDonald, T. R. Utterback, J. A. Malek, K. D. Linher, M. M. Garrett, A. M. Stewart, M. D. Cotton, M. S. Pratt, C. A. Phillips, D. Richardson, J. Heidelberg, G. G. Sutton, R. D. Fleischmann, J. A. Eisen, C. M. Fraser et al. 1999. Evidence for lateral gene transfer between Archaea and bacteria from genome sequence of Thermotoga maritima. Nature 399:323-329.

Nelson, K. E., I. T. Paulsen, J. F. Heidelberg, and C. M. Fraser. 2000. Status of genome projects for nonpathogenic bacteria and archaea. Nature Biotechnology 18:1049-1054.

Newman, D. J., G. M. Cragg, and K. M. Snader. 2000. The influence of natural products upon drug discovery. Natural Product Reports 17:215-234.

Nierman, W., J. A. Eisen, and C. M. Fraser. 2000. Microbial genome sequencing 2000: new insights into physiology, evolution and expression analysis. Research Microbiology 151:79-84.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Peng, S. X. 2000. Hyphenated HPLC-NMR and its applications in drug discovery. Biomedical Chromatography 14:430-441.

Pizza, M., V. Scarlato, V. Masignani, M. M. Giuliani, B. Arico, M. Comanducci, G. T. Jennings, L. Baldi, E. Bartolini, B. Capecchi, C. L. Galeotti, E. Luzzi, R. Manetti, E. Marchetti, M. Mora, S. Nuti, G. Ratti, L. Santini, S. Savino, M. Scarselli, E. Storni, P. Zuo, M. Broeker, E. Hundt, B. Knapp, E. Blair, T. Mason, H. Tettelin, D. W. Hood, A. C. Jeffries, N. J. Saunders, D. M. Granoff, J. C. Venter, E. R. Moxon, G. Grandi, and R. Rappuoli. 2000. Identification of vaccine candidates against serogroup B meningococcus by whole-genome sequencing. Science 287:1816-1820.

Pomponi, S. A. 1999. The bioprocess-technological potential of the sea. Journal of Biotechnology 70:5-13.


Read, T. D., S. R. Gill, H. Tettelin, and B. A. Dougherty. 2001. Finding drug targets in microbial genomes. Drug Discovery Today 6:887-892.

Rohlin, L., M. K. Oh, and J. C. Liao. 2001. Microbial pathway engineering for industrial processes: evolution, combinatorial biosynthesis and rational design. Current Opinions in Microbiology 4:330.

Rondon, M. R., P. R. August, A. D. Bettermann, S. F. Brady, T. H. Grossman, M. R. Liles, K. A. Loiacono, B. A. Lynch, I. A. MacNeil, C. Minor, C. L. Tiong, M. Gilman, M. S. Osburne, J. Clardy, J. Handelsman, and R. M. Goodman. 2000. Cloning the soil metagenome: a strategy for accessing the genetic and functional diversity of uncultured microorganisms. Applied and Environmental Microbiology 66:2541-2547.

Rossbach, M., and G. Kniewald. 1997. Concepts of marine specimen banking. Chemosphere 34:1997-2010.


Sato, T., T. Ishii, and Y. Okahata. 2001. In vitro gene delivery mediated by chitosan. Effect of pH, serum, and molecular mass of chitosan on the transfection efficiency. Biomaterials 22:2075-2080.

Saunders, N. J., A. C. Jeffries, J. F. Peden, D. W. Hood, H. Tettelin, R. Rappuoli, and E. R. Moxon. 2000. Repeat-associated phase variable genes in the complete genome sequence of Neisseriameningitidis strain MC58. Molecular Microbiology 37:207-215.

Smith, G. V., and R. L. Parr. 1998. Intellectual Property: Licensing and Joint Venture Strategies. John Wiley & Sons, Inc., New York.

Staunton, J., and B. Wilkinson. 2001. Combinatorial biosynthesis of polyketides and nonribosomal peptides. Current Opinions Chemical Biology 5:159-164.

Suh, J. K. F., and H. W. T. Matthew. 2000. Application of chitsosan-based polysaccharide biomaterials in cartilage tissue engineering: a review. Biomaterials 21:2589-2598.


Trenter, M. L., Ed. 1999. From Test Tube to Patient: Improving Health Through Human Drugs. Center for Drug Evaluation and Research Special Report. United States Food and Drug Administration. Rockville, Md.

Turner, D. M. 1996. Natural product source material use in the pharmaceutical industry: the Glaxo experience. Journal of Ethnopharmacology 51:39-43.


Ward, D. M., R. Weller, and M. M. Bateson. 1990. 16S rRNA sequences reveal numerous uncultured microorganisms in a natural community. Nature 345:63-65.

Ward, D. M., M. M. Bateson, R. Weller, and A. L. Ruff-Roberts. 1992. Ribosomal RNA analysis of microorganisms as they occur in nature. Advances in Microbial Ecology 12:219-286.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×

Weber, J. N., and E. W. White. 1973. Carbonate minerals as precursors of new ceramic, metal, and polymer materials for biomedical applications. Mineral Science Engineering 5:151-165.

Wilson, I. D. 2000. Multiple hyphenation of liquid chromatography with nuclear magnetic resonance spectroscopy, mass spectrometry and beyond. Journal of Chromatography A 892 :315-327.

Xue, Y., and D. H. Sherman. 2001. Biosynthesis and combinatorial biosynthesis of pikromycin-related macrolides in Streptomyces venezuelae. Metabolic Engineering 3:15-26.

Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
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Page 20
Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×
Page 21
Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×
Page 22
Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×
Page 23
Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×
Page 24
Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×
Page 25
Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×
Page 26
Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×
Page 27
Suggested Citation:"Biomedical Applicaions of Marine Natural Products: Overview of the 2001 Workshop." National Research Council. 2002. Marine Biotechnology in the Twenty-First Century: Problems, Promise, and Products. Washington, DC: The National Academies Press. doi: 10.17226/10340.
×
Page 28
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Dramatic developments in understanding the fundamental underpinnings of life have provided exciting opportunities to make marine bioproducts an important part of the U.S. economy. Several marine based pharmaceuticals are under active commercial development, ecosystem health is high on the public's list of concerns, and aquaculture is providing an ever greater proportion of the seafood on our tables. Nevertheless, marine biotechnology has not yet caught the public's, or investor's, attention. Two workshops, held in October 1999 and November 2001 at the National Academies, were successful in highlighting new developments and opportunities in environmental and biomedical applications of marine biotechnology, and also in identifying factors that are impeding commercial exploitation of these products. This report includes a synthesis of the 2001 sessions addressing drug discovery and development, applications of genomics and proteomics to marine biotechnology, biomaterials and bioengineering, and public policy and essays contributed by the workshop speakers.

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