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Dr. Harshad Malve
Marine Pharmacology:
Deals with investigation, identification & use of medically
important plants & animals, extracts or substances isolated
from marine organisms
With an estimated 75% of earth’s surface covered by water,
research into the chemistry of marine organisms is
unexplored & represents a vast resource for new drugs to
combat major diseases such as cancer, AIDS or malaria.
A wide variety of environments
Biodiversity
The oceans are our most biodiverse environment with 34
of the 36 known phyla represented
By comparison, the land has only 17 of the known Phyla!
Genetic diversity translates to chemical diversity =
Promising new drugs
Research typically focuses on slow moving or sessile
organisms because of their inherent need for chemical
defenses
Marine pharmacologists work
with extracts or substances
isolated from marine organisms
Cont.
Sources of Marine drugs
Majority of marine products have been isolated from:
Sponges
Coelenterates (sea whips, sea fans and soft corals)
 Tunicates
Opisthobranch molluscs (nudibranchs, sea hares, etc.)
Echinoderms (starfish, sea cucumbers, etc.)
Bryozoans (moss animals)
A wide variety of marine microorganisms in their tissues
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Development of Marine pharmacology
Late 1970s: Marine drug discovery begun, early
investigators demonstrated marine plants & animals were
genetically & biochemically unique
In the 1970's, in a survey of Caribbean invertebrates, the
impressive cytotoxic properties of extracts of mangrove
ascidian Ecteinascidia turbinata were discovered
After 20 years of advancements in chemistry, the active
substances, named the ecteinascidins were isolated in
1990
Cont.
Drugs of marine origin:
Ziconotide
1st
drug of marine origin which obtained
approval by the FDA on December 31st
2004
A non-opioid, non-NSAID, non-local anesthetic used for
amelioration of chronic pain
Derived from the toxin of cone snail Conus magus
Contains synthetic form of the cone snail peptide ω-
conotoxin
Blocks the N-Type calcium channels on the primary
nociceptive nerves in the spinal cord
Used only for “management of severe chronic pain”
Approved for the treatment of chronic pain as a morphine
replacement therapy
It is the most powerful painkiller known to date
Must be administered intrathecally
Common side effects: dizziness, nausea, confusion &
headache
Rare side effects: hallucinations, suicidal thoughts, new or
worsening depression, meningitis and seizures
Cont.
Anti-cancer candidates
Ecteinascidin 743
Didemnin B
Dolastatin 10
Halichondrin B
Bryostatin 1
Aplidin (APL)
Kahalalide F (KF)
Ecteinascidin 743
A tetrahydroisoquinoline alkaloid produced by the
tunicate Ecteinascidia turbinata
Chemically related to a rare group of microbial
antibiotics, the saframycins
Induces a broad inhibition of activated transcription with
no effect on the constitutive transcription
Cont.
Dose limiting toxicities are bone marrow toxicity & fatigue
Does not induce hair loss, mucositis, neurotoxicity or
diarrhoea
European Union & US FDA have granted orphan drug
status for the treatment of patients with advanced soft
tissue sarcoma & ovarian cancer
It is also undergoing clinical trials for the treatment of
breast, prostate, and paediatric sarcomas
Didemnin B
Cyclodepsipeptide compounds isolated from a
tunicate (sea-squirt) Trididemhum solidum
1st
isolated in 1978 at the University of Illinois
A strong antiviral agent against both DNA and RNA viruses
like Herpes simplex virus type 1
Cont.
A strong immunosuppressant that shows some potential
in skin graft
Showed impressive cytotoxicity against lymphomas
It has completed phase II human clinical trials against
adenocarcinoma of the kidney
Dolastin-10
A pentapeptide derived from marine mollusk Dolabella
auricularia with potential antineoplastic activity
Showed outstanding inhibitory effects against several
forms of skin cancers in laboratory studies
Binding to tubulin, it inhibits microtubule assembly,
resulting in the formation of tubulin aggregates &
inhibition of mitosis
Also induces tumor cell apoptosis through a mechanism
involving bcl-2
Halichondrin B
This metabolite was discovered in the
marine sponge Halichondria okadai in 1985
Highly potent cytotoxic agent
Eisai 7389 is a synthetic macrocyclic ketone derivative of
the marine natural product Halichondrin B
Entered phase I clinical trials in 2002 & has recently
progressed to phase II clinical trials for the treatment of
advanced and metastatic breast cancer
Bryostatin-1
A macrolactone isolated from the
marine bryozoan, Bugula neritina
Modulates cell-signaling enzyme protein kinase C (PKC)
activity
It binds to & inhibits the enzyme resulting in the
inhibition of tumor cell proliferation, the promotion of
tumor cell differentiation & the induction of tumor cell
apoptosis
Sensitizes cancer cells to cytotoxic effects of anti-cancer
agents & act synergistically with other chemotherapeutic
agents
Chronic activation of PKC isozymes with bryostatin-1 induces
synthesis of the proteins that are involved in memory
consolidation & therefore, may represent a pharmacological
strategy for antidementic & memory enhancement therapies
Cont.
In phase I studies, tumour responses have been observed
in patients with malignant melanoma, lymphoma &
ovarian carcinoma
Dose-limiting toxicity is myalgias
Cont.
Aplidin (APL)
A cyclic depsipeptide isolated from the Mediterranean
tunicate Aplidium albicans
Has a potent activity against human MM cell lines &
primary MM tumor cells, including cells resistant to
conventional or novel anti-MM agents
Decreases the secretion of the Vascular Endothelial Growth
factor (VEGF) & expression of the VEGF-r1 receptor
Induces apoptosis via activation of Jun N-terminal kinase,
increases intracellular production of ROS & alters
mitochondrial membrane potential
Blocks the cell cycle progression at G1
A remarkable lack of haematological toxicity
6th
October, 2004: Orphan drug status by the US FDA for
the treatment of Multiple Myeloma (MM)
FDA approves production process strategy of Aplidin(R),
as an Anti-tumor agent in 2008
Cont.
Kahalalide F (KF)
One of the families of natural depsipeptides isolated from
Hawaiian herbivorous marine mollusk Elysia rufescens
Potent cytotoxic activity in vitro against cell lines from solid
tumors including prostate, breast & colon carcinomas,
neuroblastoma, chondrosarcoma & osteosarcoma
Mechanism of KF action is mostly unknown
Seems to have the lysosomes as the cellular target
Cont.
Dose limiting toxicity is acute transaminitis (raised ALT &
AST), with a remarkable absence of bone marrow
suppression, alopecia & other organ toxicities
Phase I trials demonstrated safety of Kahalalide F in
Prostate Cancer patients
Amphilactams A–S
Geodin A
Anti-helmintics
Amphilactams A–S
Macrocyclic lactone/lactams isolated from the sponge
Amphimedon spp. showed antihelmintic acrivity
comparable to that of existing anthelmintics like levamisole
& closantel
But the mechanism of action of these compounds was not
determined
Geodin A
Geodin A Mg salt, was isolated from the sponge Geodia sp.
Mechanism of action of the pure Geodin A was not
explored
It occurs naturally as the Mg salt
It was nematocidal to the nematode Haemonchus
contortus
Loloatins A–D
Myticin
Psammaplin A
Anti-bacterials
Loloatins A–D
Cyclic decapeptides isolated from a marine bacterium
Exhibited in vitro antimicrobial activity against
methicillin-resistant Staphylococcus aureus, vancomycin-
resistant enterococci & penicillin-resistant Streptococcus
pneumoniae
Myticin
Isolated from hemocytes & plasma of the mussel Mytilus
galloprovincialis
Myticins A & B had marked activity against the Gram-
positive strains Micrococcus luteus, Bacillus megaterium &
Enterococcus viridans, other Gram-positive, Gram-
negative bacteria & fungi were unaffected
Psammaplin A
A bromotyrosine derivative from the sponge
Psammaplysilla sp. possessed antibacterial activity against
methicillin-resistant Gram-positive Staphylococcus aureus
Monoterpenes
Isolated from the marine red alga Plocamium hamatum
One of them was antitubercular towards
Mycobacterium tuberculosis & Mycobacterium avium
Anti-tubercular
 Bengazole, bengamide
 Oceanapiside
 Spongistatin I
 Tanikolide
 Theopederins F–J
Anti-fungals
The bengazole derivatives & a new bengamide obtained
from the sponge Pachastrissa sp
The bengazole derivatives were observed to be active
against Candida albicans
Oceanapiside, from the sponge Oceanapia phillipensis,
demonstrated antifungal activity against the fluconazole-
resistant yeast Candida glabrata
Cont.
Spongistatin 1 isolated from the sponge Hyrtios erecta
demonstrated potent microtubule-severing activity
Mechanism of action of was significantly differerent from
all other antimicrotubule agents
Tanikolide was isolated from the marine cyanobacterium
Lyngbia majuscula
Theopederins F–J from the sponge Theonella swinhoei
Theopederin-F was particularly effective against
Saccharomyces cerevisiae
Cont.
15-a-Methoxy- puupehenol
Isolated from the marine sponge Hyrtios sp. demonstrated
antimalarial activity against chloroquine-susceptible &
chloroquine-resistant strains of P. falciparum
Anti-malarials
 Lamellarin α-20-sulfate
 Papuamides A–D
 Polycitone A
 Glycosaminoglycan
 Sulfated β-galactan
 Poly-hydroxysteroids
 Sansalvamide
Anti-virals
Alkaloid lamellarin α 20-sulfate in an unidentified ascidian
showed selective in vitro inhibition of HIV integrase
Papuamides A, B, C & D were isolated from the sponges
Theonella mirabilis & Theonella swinhoei
Papuamides A & B inhibited the infection of human T-
lymphoblastoid cells by HIV-1 in vitro
Cont.
Polycitone A isolated from the ascidian Polyctor sp., is a
potent inhibitor of the reverse transcriptase of HIV & both
C and B retroviruses, as well as a general inhibitor of
cellular DNA polymerases
As polycitone A is a general inhibitor of DNA polymerases
it cannot serve as an anti-HIV drug but structural
modifications of polycitone A could lead towards the
rational design of new derivatives with anti-HIV reverse
transcriptase activity
Cont.
Synthesis of sulfated derivatives of a glycosaminoglycan
isolated from the marine bacterium Pseudomonas sp. & act
against two strains of influenza virus types A & but not B
Introduction of sulfate groups into polysaccharides
containing L-glutamic acid resulted in antiviral activity
against influenza virus type A, but not against type B, this
activity was similar to that of ribavirin
Cont.
Sulfated β-galactan from the marine clam Meretrix
petechialis inhibited CD4 HeLa cells from forming syncytia
It was interpreted as probably the result of a “direct
interaction of the polysaccharide with the HIV binding
site at the membrane protein receptor CD4’’
Cont.
Maitotoxin
A marine toxin causing ciguatera poisoning
Mechanism of action was similar to U46619 - a
thromboxane A receptor agonist
Anti-plateletes
Sulfated fucans:
Derived from brown algae & echinoderm
Highly branched sulfated fucans from brown algae
directly inhibited thrombin,
Linear fucans from echinoderms required the presence of
antithrombin or heparin cofactor II for inhibition of
thrombin
Anti-Coagulants
Anti-inflammatory
Africanene,
Cacospongiolide B,
Palinurin, Palinurine A and B
Plakotenin
Africanene
Sesquiterpene africanene, isolated from the soft coral
Sinularia leptoclados
It resulted in a more potent reduction of paw volume than
that produced by 100 mg/kg body weight of ibuprofen, in
carrageenan-induced rat edema assay
Cacospongionolide B
A novel sesterterpene inhibitor of human synovial
phospholipase A2 isolated from the sponge Fasciospongia
cavernosa
It irreversibly inhibited both secretory PLA2 in vitro and
group II secretory PLA2in vivo
Palinurin, Palinurine A & B
Isolated from the marine sponge Ircinia echinata
Palinurin inhibited TXB2& Oxide radicals
Palinurine A and B were relatively ineffective inhibitors of
both TXB2and Oxide radicals
Immunosuppressants
Immunosuppresant activity was reported for the
novel glycolipids simplexides, isolated from the
sponge Plakortis simplex
Showed a 43% inhibitory effect on lymph node cell
proliferation
Limiting factors for development of
marine drugs
Supply (sustainable, industrially feasible)
Formulation (suitable for clinical use)
Analytical method & preclinical PKs
Pharmacogenetics (metabolic pathway)
Therapeutic index
Toxicities (Xeno)
Measures to maintain supply
Controlled & sustainable use of natural resources
Mariculture: Favouring (by farming) the growth of the
organism in its natural milieu
Aquaculture: Culture of the organism under artificial
conditions
Hemisynthesis: use of a parent/related compound as the
starting point followed by a short/industrially effective
synthetic process
Synthesis
The available data demonstrates
that:
“The marine ecosystem is not only
productive to discover novel entities
but it is also a tool to identify new
cellular targets for therapeutic
intervention”
Marine pharmacology By Dr. Harshad Malve

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Marine pharmacology By Dr. Harshad Malve

  • 2. Marine Pharmacology: Deals with investigation, identification & use of medically important plants & animals, extracts or substances isolated from marine organisms With an estimated 75% of earth’s surface covered by water, research into the chemistry of marine organisms is unexplored & represents a vast resource for new drugs to combat major diseases such as cancer, AIDS or malaria.
  • 3. A wide variety of environments
  • 4. Biodiversity The oceans are our most biodiverse environment with 34 of the 36 known phyla represented By comparison, the land has only 17 of the known Phyla! Genetic diversity translates to chemical diversity = Promising new drugs
  • 5. Research typically focuses on slow moving or sessile organisms because of their inherent need for chemical defenses Marine pharmacologists work with extracts or substances isolated from marine organisms Cont.
  • 6. Sources of Marine drugs Majority of marine products have been isolated from: Sponges Coelenterates (sea whips, sea fans and soft corals)  Tunicates Opisthobranch molluscs (nudibranchs, sea hares, etc.) Echinoderms (starfish, sea cucumbers, etc.) Bryozoans (moss animals) A wide variety of marine microorganisms in their tissues
  • 8. Development of Marine pharmacology
  • 9. Late 1970s: Marine drug discovery begun, early investigators demonstrated marine plants & animals were genetically & biochemically unique In the 1970's, in a survey of Caribbean invertebrates, the impressive cytotoxic properties of extracts of mangrove ascidian Ecteinascidia turbinata were discovered After 20 years of advancements in chemistry, the active substances, named the ecteinascidins were isolated in 1990 Cont.
  • 10. Drugs of marine origin:
  • 11.
  • 12.
  • 13.
  • 14. Ziconotide 1st drug of marine origin which obtained approval by the FDA on December 31st 2004 A non-opioid, non-NSAID, non-local anesthetic used for amelioration of chronic pain Derived from the toxin of cone snail Conus magus Contains synthetic form of the cone snail peptide ω- conotoxin Blocks the N-Type calcium channels on the primary nociceptive nerves in the spinal cord
  • 15. Used only for “management of severe chronic pain” Approved for the treatment of chronic pain as a morphine replacement therapy It is the most powerful painkiller known to date Must be administered intrathecally Common side effects: dizziness, nausea, confusion & headache Rare side effects: hallucinations, suicidal thoughts, new or worsening depression, meningitis and seizures Cont.
  • 16. Anti-cancer candidates Ecteinascidin 743 Didemnin B Dolastatin 10 Halichondrin B Bryostatin 1 Aplidin (APL) Kahalalide F (KF)
  • 17. Ecteinascidin 743 A tetrahydroisoquinoline alkaloid produced by the tunicate Ecteinascidia turbinata Chemically related to a rare group of microbial antibiotics, the saframycins Induces a broad inhibition of activated transcription with no effect on the constitutive transcription
  • 18. Cont. Dose limiting toxicities are bone marrow toxicity & fatigue Does not induce hair loss, mucositis, neurotoxicity or diarrhoea European Union & US FDA have granted orphan drug status for the treatment of patients with advanced soft tissue sarcoma & ovarian cancer It is also undergoing clinical trials for the treatment of breast, prostate, and paediatric sarcomas
  • 19. Didemnin B Cyclodepsipeptide compounds isolated from a tunicate (sea-squirt) Trididemhum solidum 1st isolated in 1978 at the University of Illinois A strong antiviral agent against both DNA and RNA viruses like Herpes simplex virus type 1
  • 20. Cont. A strong immunosuppressant that shows some potential in skin graft Showed impressive cytotoxicity against lymphomas It has completed phase II human clinical trials against adenocarcinoma of the kidney
  • 21. Dolastin-10 A pentapeptide derived from marine mollusk Dolabella auricularia with potential antineoplastic activity Showed outstanding inhibitory effects against several forms of skin cancers in laboratory studies Binding to tubulin, it inhibits microtubule assembly, resulting in the formation of tubulin aggregates & inhibition of mitosis Also induces tumor cell apoptosis through a mechanism involving bcl-2
  • 22. Halichondrin B This metabolite was discovered in the marine sponge Halichondria okadai in 1985 Highly potent cytotoxic agent Eisai 7389 is a synthetic macrocyclic ketone derivative of the marine natural product Halichondrin B Entered phase I clinical trials in 2002 & has recently progressed to phase II clinical trials for the treatment of advanced and metastatic breast cancer
  • 23. Bryostatin-1 A macrolactone isolated from the marine bryozoan, Bugula neritina Modulates cell-signaling enzyme protein kinase C (PKC) activity It binds to & inhibits the enzyme resulting in the inhibition of tumor cell proliferation, the promotion of tumor cell differentiation & the induction of tumor cell apoptosis
  • 24. Sensitizes cancer cells to cytotoxic effects of anti-cancer agents & act synergistically with other chemotherapeutic agents Chronic activation of PKC isozymes with bryostatin-1 induces synthesis of the proteins that are involved in memory consolidation & therefore, may represent a pharmacological strategy for antidementic & memory enhancement therapies Cont.
  • 25. In phase I studies, tumour responses have been observed in patients with malignant melanoma, lymphoma & ovarian carcinoma Dose-limiting toxicity is myalgias Cont.
  • 26. Aplidin (APL) A cyclic depsipeptide isolated from the Mediterranean tunicate Aplidium albicans Has a potent activity against human MM cell lines & primary MM tumor cells, including cells resistant to conventional or novel anti-MM agents Decreases the secretion of the Vascular Endothelial Growth factor (VEGF) & expression of the VEGF-r1 receptor
  • 27. Induces apoptosis via activation of Jun N-terminal kinase, increases intracellular production of ROS & alters mitochondrial membrane potential Blocks the cell cycle progression at G1 A remarkable lack of haematological toxicity 6th October, 2004: Orphan drug status by the US FDA for the treatment of Multiple Myeloma (MM) FDA approves production process strategy of Aplidin(R), as an Anti-tumor agent in 2008 Cont.
  • 28. Kahalalide F (KF) One of the families of natural depsipeptides isolated from Hawaiian herbivorous marine mollusk Elysia rufescens Potent cytotoxic activity in vitro against cell lines from solid tumors including prostate, breast & colon carcinomas, neuroblastoma, chondrosarcoma & osteosarcoma Mechanism of KF action is mostly unknown Seems to have the lysosomes as the cellular target
  • 29. Cont. Dose limiting toxicity is acute transaminitis (raised ALT & AST), with a remarkable absence of bone marrow suppression, alopecia & other organ toxicities Phase I trials demonstrated safety of Kahalalide F in Prostate Cancer patients
  • 31. Amphilactams A–S Macrocyclic lactone/lactams isolated from the sponge Amphimedon spp. showed antihelmintic acrivity comparable to that of existing anthelmintics like levamisole & closantel But the mechanism of action of these compounds was not determined
  • 32. Geodin A Geodin A Mg salt, was isolated from the sponge Geodia sp. Mechanism of action of the pure Geodin A was not explored It occurs naturally as the Mg salt It was nematocidal to the nematode Haemonchus contortus
  • 34. Loloatins A–D Cyclic decapeptides isolated from a marine bacterium Exhibited in vitro antimicrobial activity against methicillin-resistant Staphylococcus aureus, vancomycin- resistant enterococci & penicillin-resistant Streptococcus pneumoniae
  • 35. Myticin Isolated from hemocytes & plasma of the mussel Mytilus galloprovincialis Myticins A & B had marked activity against the Gram- positive strains Micrococcus luteus, Bacillus megaterium & Enterococcus viridans, other Gram-positive, Gram- negative bacteria & fungi were unaffected
  • 36. Psammaplin A A bromotyrosine derivative from the sponge Psammaplysilla sp. possessed antibacterial activity against methicillin-resistant Gram-positive Staphylococcus aureus
  • 37. Monoterpenes Isolated from the marine red alga Plocamium hamatum One of them was antitubercular towards Mycobacterium tuberculosis & Mycobacterium avium Anti-tubercular
  • 38.  Bengazole, bengamide  Oceanapiside  Spongistatin I  Tanikolide  Theopederins F–J Anti-fungals
  • 39. The bengazole derivatives & a new bengamide obtained from the sponge Pachastrissa sp The bengazole derivatives were observed to be active against Candida albicans Oceanapiside, from the sponge Oceanapia phillipensis, demonstrated antifungal activity against the fluconazole- resistant yeast Candida glabrata Cont.
  • 40. Spongistatin 1 isolated from the sponge Hyrtios erecta demonstrated potent microtubule-severing activity Mechanism of action of was significantly differerent from all other antimicrotubule agents Tanikolide was isolated from the marine cyanobacterium Lyngbia majuscula Theopederins F–J from the sponge Theonella swinhoei Theopederin-F was particularly effective against Saccharomyces cerevisiae Cont.
  • 41. 15-a-Methoxy- puupehenol Isolated from the marine sponge Hyrtios sp. demonstrated antimalarial activity against chloroquine-susceptible & chloroquine-resistant strains of P. falciparum Anti-malarials
  • 42.  Lamellarin α-20-sulfate  Papuamides A–D  Polycitone A  Glycosaminoglycan  Sulfated β-galactan  Poly-hydroxysteroids  Sansalvamide Anti-virals
  • 43. Alkaloid lamellarin α 20-sulfate in an unidentified ascidian showed selective in vitro inhibition of HIV integrase Papuamides A, B, C & D were isolated from the sponges Theonella mirabilis & Theonella swinhoei Papuamides A & B inhibited the infection of human T- lymphoblastoid cells by HIV-1 in vitro Cont.
  • 44. Polycitone A isolated from the ascidian Polyctor sp., is a potent inhibitor of the reverse transcriptase of HIV & both C and B retroviruses, as well as a general inhibitor of cellular DNA polymerases As polycitone A is a general inhibitor of DNA polymerases it cannot serve as an anti-HIV drug but structural modifications of polycitone A could lead towards the rational design of new derivatives with anti-HIV reverse transcriptase activity Cont.
  • 45. Synthesis of sulfated derivatives of a glycosaminoglycan isolated from the marine bacterium Pseudomonas sp. & act against two strains of influenza virus types A & but not B Introduction of sulfate groups into polysaccharides containing L-glutamic acid resulted in antiviral activity against influenza virus type A, but not against type B, this activity was similar to that of ribavirin Cont.
  • 46. Sulfated β-galactan from the marine clam Meretrix petechialis inhibited CD4 HeLa cells from forming syncytia It was interpreted as probably the result of a “direct interaction of the polysaccharide with the HIV binding site at the membrane protein receptor CD4’’ Cont.
  • 47. Maitotoxin A marine toxin causing ciguatera poisoning Mechanism of action was similar to U46619 - a thromboxane A receptor agonist Anti-plateletes
  • 48. Sulfated fucans: Derived from brown algae & echinoderm Highly branched sulfated fucans from brown algae directly inhibited thrombin, Linear fucans from echinoderms required the presence of antithrombin or heparin cofactor II for inhibition of thrombin Anti-Coagulants
  • 50. Africanene Sesquiterpene africanene, isolated from the soft coral Sinularia leptoclados It resulted in a more potent reduction of paw volume than that produced by 100 mg/kg body weight of ibuprofen, in carrageenan-induced rat edema assay
  • 51. Cacospongionolide B A novel sesterterpene inhibitor of human synovial phospholipase A2 isolated from the sponge Fasciospongia cavernosa It irreversibly inhibited both secretory PLA2 in vitro and group II secretory PLA2in vivo
  • 52. Palinurin, Palinurine A & B Isolated from the marine sponge Ircinia echinata Palinurin inhibited TXB2& Oxide radicals Palinurine A and B were relatively ineffective inhibitors of both TXB2and Oxide radicals
  • 53. Immunosuppressants Immunosuppresant activity was reported for the novel glycolipids simplexides, isolated from the sponge Plakortis simplex Showed a 43% inhibitory effect on lymph node cell proliferation
  • 54. Limiting factors for development of marine drugs Supply (sustainable, industrially feasible) Formulation (suitable for clinical use) Analytical method & preclinical PKs Pharmacogenetics (metabolic pathway) Therapeutic index Toxicities (Xeno)
  • 55. Measures to maintain supply Controlled & sustainable use of natural resources Mariculture: Favouring (by farming) the growth of the organism in its natural milieu Aquaculture: Culture of the organism under artificial conditions Hemisynthesis: use of a parent/related compound as the starting point followed by a short/industrially effective synthetic process Synthesis
  • 56. The available data demonstrates that: “The marine ecosystem is not only productive to discover novel entities but it is also a tool to identify new cellular targets for therapeutic intervention”

Notas del editor

  1. in patients for whom intrathecal (IT) therapy is warranted and who are intolerant of or refractory to other treatment, such as systemic analgesics, adjunctive therapies or IT morphine
  2. n cell biology, a constitutively active protein is a protein whose activity is constant and active
  3. Inhibits the activation of the multidrug resistant pathway that is considered to be the main mechanism of primary and acquired resistance of cancer cells to natural drugs such doxorubicin and taxanes
  4. Orphan drug designation is awarded to drugs that offer potential therapeutic value in the treatment of rare diseases and conditions and therefore may benefit directly from the provisions of the Orphan Act which includes: regulatory assistance and numerous financial incentives for the development and approval of the orphan product, including seven years of marketing exclusivity; New Drug Application fee waivers; tax credits for clinical research and grant funding for the investigation of the rare disease treatment.
  5. these investigators noted that the aglycon exerted higher antifungal activity than the glycoside, possibly due to better cell penetration
  6. that was interpreted as probably the result of a ‘direct interaction of the polysaccharide with the HIV binding site at the membrane protein receptor CD4’’.
  7. Ciguatera: Ciguatera is a foodborne illness poisoning in humans caused by eating marine species whose flesh is contaminated with a toxin known as ciguatoxin, which is present in many microorganisms (particularly the micro-alga Gambierdiscus toxicus) living in tropical waters.
  8. A critical step is the incorporation of a sustainable supply, in order to ensure a sequential pathway of preclinical-clinical investigations. Complexity of the chemical structures generally seen in marine derived compounds can limit the development of synthesis processes. major advances in the aquaculture of marine microorganisms and synthesis of complex molecules are needed to facilitate the incorporation of additional candidates to the development track Additional factors such as the identification of a feasible clinical formulation, investigation of the metabolic pathways and preclinical evaluation of new toxicological models have to be considered instrumental, clearly implying the need of an interdisciplinary team involving experts from many different areas of research