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Title: Tetrodotoxin  
Author: World Heritage Encyclopedia
Language: English
Subject: Huwentoxin, Taricha, California newt, Epibatidine, Vanillotoxin
Collection: Alcohols, Biological Toxin Weapons, Guanidines, Ion Channel Toxins, Neurotoxins, Sodium Channel Blockers, Vertebrate Toxins
Publisher: World Heritage Encyclopedia


IUPAC name
Other names
anhydrotetrodotoxin, 4-epitetrodotoxin, tetrodonic acid, TTX
ChemSpider  N
Jmol-3D images Image
Molar mass 319.268
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
 N  (: Y/N?)

Tetrodotoxin, frequently abbreviated as TTX, is a potent neurotoxin. Its name derives from Tetraodontiformes, an order that includes pufferfish, porcupinefish, ocean sunfish or mola, and triggerfish; several species that carry the toxin. Although tetrodotoxin was discovered in these fish and found in several other animals (e.g., blue-ringed octopus, rough-skinned newt,[1] and Naticidae[2]) it is actually produced by certain symbiotic bacteria, such as Pseudoalteromonas tetraodonis, certain species of Pseudomonas and Vibrio, as well as some others that reside within these animals.

Tetrodotoxin inhibits the firing of action potentials in nerves by binding to the voltage-gated sodium channels in nerve cell membranes and blocking the passage of sodium ions (responsible for the rising phase of an action potential) into the nerve cell.[3][4]

Its mechanism of action, selective blocking of the sodium channel, was shown definitively in 1964 by Toshio Narahashi and professor John W. Moore at Duke University, using the sucrose gap voltage clamp technique.[5]


  • Sources in nature 1
  • Biochemistry 2
  • Chemical synthesis 3
  • Poisoning 4
    • Toxicity 4.1
    • History 4.2
    • Symptoms and treatment 4.3
    • Geographic frequency of toxicity 4.4
    • Food analysis 4.5
    • Detection in body fluids 4.6
  • Modern therapeutic research 5
  • Regulation 6
  • Popular culture 7
  • See also 8
  • References 9
  • External links 10

Sources in nature

Tetrodotoxin has been isolated from widely differing animal species, including western newts of the genus Taricha (where it was formerly termed "tarichatoxin"), pufferfish, toads of the genus Atelopus, several species of the blue-ringed octopus of the genus Hapalochlaena (where it was called "maculotoxin"), several sea stars, certain angelfish, a polyclad flatworm, land planarians of the genus Bipalium,[6] several species of Chaetognatha (arrow worms), several nemerteans (ribbonworms) and several species of xanthid crabs.[7] The toxin is variously used as a defensive biotoxin to ward off predation, or as both a defensive and predatory venom (octopi, chaetognaths and ribbonworms). Even though the toxin acts as a defense mechanism, some predators such as the common garter snake have developed a resistance to TTX, which allows them to prey upon toxic newts.[8] Tarichatoxin and maculotoxin were shown to be identical to tetrodotoxin in 1964 (Mosher et al.)[9] and 1978,[10] respectively. The toxin is produced by bacteria within blue-ringed octopi.[11] The most common bacteria associated with TTX production are Vibrio bacteria, with Vibrio alginolyticus being the most common species. Pufferfish,[12] chaetognaths,[13] and nemerteans[14] have been shown to contain Vibrio alginolyticus and TTX. The link between these facts and production of TTX in animals has not been firmly established, and there remains much debate in literature as to whether the bacteria are truly the source of TTX in animals.[7]


Tetrodotoxin binds to what is known as site 1 of the fast voltage-gated sodium channel.[15] Site 1 is located at the extracellular pore opening of the ion channel. The binding of any molecules to this site will temporarily disable the function of the ion channel. Saxitoxin, neosaxitoxin and several of the conotoxins also bind the same site.

The use of this toxin as a biochemical probe has elucidated two distinct types of voltage-gated sodium channels present in humans: the tetrodotoxin-sensitive voltage-gated sodium channel (TTX-s Na+ channel) and the tetrodotoxin-resistant voltage-gated sodium channel (TTX-r Na+ channel). Tetrodotoxin binds to TTX-s Na+ channels with a binding affinity of 5-15 nM, while the TTX-r Na+ channels bind TTX with low micromolar affinity.[16] Nerve cells containing TTX-r Na+ channels are located primarily in cardiac tissue, while nerve cells containing TTX-s Na+ channels dominate the rest of the body. The prevalence of TTX-s Na+ channels in the central nervous system makes tetrodotoxin a valuable agent for the silencing of neural activity within a cell culture.

Chemical synthesis

In 1964 a team of Scientists led by Robert B. Woodward at Harvard University elucidated the structure of tetrodotoxin.[17] Yoshito Kishi et al. Nagoya University, Nagoya, Japan, (now at Harvard University) reported the first total synthesis of D,L-tetrodotoxin in 1972.[18][19] M. Isobe et al. at Nagoya University, Japan[20][21][22] and J. Du Bois et al. at Stanford University, U.S., reported the asymmetric total synthesis of tetrodotoxin in 2003.[23] The two 2003 syntheses used very different strategies, with Isobe's route based on a Diels-Alder approach and Du Bois's work using C-H bond activation. Since then, methods have rapidly advanced, with several new strategies for the synthesis of tetrodotoxin having been developed.[24][25]



TTX is extremely toxic. The Material Safety Data Sheet for TTX lists the oral median lethal dose (LD50) for mice as 334 μg per kg.[26] For comparison, the oral LD50 of potassium cyanide for mice is 8.5 mg per kg,[27] demonstrating that even orally, TTX is more poisonous than cyanide. TTX is even more dangerous if injected; the amount needed to reach a lethal dose by injection only 8 μg per kg in mice.[28]

The toxin can enter the body of a victim by ingestion, injection, or inhalation, or through abraded skin.[29]

Poisoning occurring as a consequence of consumption of fish from the order pufferfish can contain levels of tetrodotoxin sufficient to produce the described paralysis of the diaphragm and corresponding death due to respiratory failure.[30] Toxicity varies between species and at different seasons and geographic localities, and the flesh of many pufferfish may not be dangerously toxic.[31]

The mechanism of toxicity is through the blockage of fast voltage-gated sodium channels, which are required for the normal transmission of signals between the body and brain.[32] As a result, TTX causes loss of sensation, and paralysis of voluntary muscles including the diaphragm and intercostal muscles, stopping breathing.


A Chinese Pharmacopoeia

The therapeutic use of puffer fish (tetraodon) eggs was mentioned in the first Chinese pharmacopea (Pen-T’ so Ching, The Book of Herbs, allegedly 2838-2698 BC by Shénnóng Běn Cǎo Jīng; but a later date is more likely), where they were classified as having ‘medium’ toxicity, but could have a tonic effect when used at the correct dose. The principle use was “to arrest convulsive diseases”.[33] In the Pen-T’ so Kang Mu (Index Herbacea or The Great Herbal by Li Shih-Chen, 1596) some types of the fish Ho-Tun (the current Chinese name for tetraodon) were also recognized as both toxic and (at the right dose) could be used to prepare a tonic. Increased toxicity in Ho-Tun was noted in fish caught at sea (rather than river) after the month of March. It was recognized that the most poisonous parts were the liver and eggs, but that toxicity could be reduced by soaking the eggs,[33] noting that tetrodotoxin is slightly water soluble, and soluble at 1 mg/mL in slightly acidic solutions.[34]

The Dutch physician Engelbert Kaempfer, in his "A History of Japan" (translated and published in English in 1727), described how well known the toxic effects of the fish were, to the extent that it would be used for suicide and that the Emperor specifically decreed that soldiers were not permitted to eat it. There is also evidence from other sources that knowledge of such toxicity was widespread throughout south-East Asia and India.[33]

The first recorded cases of TTX poisoning affecting Westerners are from the logs of Captain James Cook from 7 September 1774.[30] On that date Cook recorded his crew eating some local tropic fish (pufferfish), then feeding the remains to the pigs kept on board. The crew experienced numbness and shortness of breath, while the pigs were all found dead the next morning. In hindsight, it is clear that the crew survived a mild dose of tetrodotoxin, while the pigs ate the pufferfish body parts that contain most of the toxin, thus being fatally poisoned.

The toxin was first isolated and named in 1909 by Japanese scientist Dr. Yoshizumi Tahara.[30]

Symptoms and treatment

The diagnosis of pufferfish poisoning is based on the observed symptamatology and recent dietary history.[35]

Symptoms typically develop within 30 minutes of ingestion, but may be delayed by up to four hours; however, if the dose is fatal, symptoms are usually present within 17 minutes of ingestion.[30] Paresthesia of the lips and tongue is followed by hypersalivation, sweating, headache, weakness, lethargy, incoordination, tremor, paralysis, cyanosis, aphonia, dysphagia, and seizures. The gastrointestinal symptoms are often severe and include nausea, vomiting, diarrhea, and abdominal pain; death is usually secondary to respiratory failure.[35] There is increasing respiratory distress, speech is affected, and the victim usually exhibits dyspnea, cyanosis, and hypotension. Paralysis increases, and convulsions, mental impairment, and cardiac arrhythmia may occur. The victim, although completely paralyzed, may be conscious and in some cases completely lucid until shortly before death, which generally occurs within 4 to 6 hours (range ~20 minutes to ~8 hours).[36]

If the patient survives 24 hours, recovery without any residual effects will usually occur over a few days.[35]

Therapy is supportive and based on symptoms, with aggressive early airway management.[30] If ingested, treatment can consist of emptying the stomach, feeding the victim activated charcoal to bind the toxin, and taking standard life-support measures to keep the victim alive until the effect of the poison has worn off.[30] Alpha adrenergic agonists are recommended in addition to intravenous fluids to combat hypotension; anticholinesterase agents "have been proposed as a treatment option but have not been tested adequately".[36]

No antidote has been developed and approved for human use, but a primary research report (preliminary result) indicates that a monoclonal antibody specific to tetrodotoxin is in development by USAMRIID that was effective, in the one study, for reducing toxin lethality in tests on mice.[37]

Geographic frequency of toxicity

Poisonings from tetrodotoxin have been almost exclusively associated with the consumption of pufferfish from waters of the Indo-Pacific ocean regions, but pufferfishes from other regions are much less commonly eaten. Several reported cases of poisonings, including fatalities, involved pufferfish from the Atlantic Ocean, Gulf of Mexico, and Gulf of California. There have been no confirmed cases of tetrodotoxicity from the Atlantic pufferfish, Sphoeroides maculatus, but in three studies, extracts from fish of this species were highly toxic in mice. Several recent intoxications from these fishes in Florida were due to saxitoxin, which causes paralytic shellfish poisoning with very similar symptoms and signs. The trumpet shell Charonia sauliae has been implicated in food poisonings, and evidence suggests it contains a tetrodotoxin derivative. There have been several reported poisonings from mislabelled pufferfish, and at least one report of a fatal episode in Oregon when an individual swallowed a rough-skinned newt Taricha granulosa.[38]

In 2009, a major scare in the Auckland Region of New Zealand was sparked after several dogs died eating Pleurobranchaea maculata (grey side-gilled seaslug) on beaches.[39] Children and pet owners were asked to avoid beaches, and recreational fishing was also interrupted for a time. After exhaustive analysis, it was found that the sea slugs must have ingested tetrodotoxin.[40]

Statistical factors

Statistics from the Tokyo Bureau of Social Welfare and Public Health indicate 20–44 incidents of fugu poisoning per year between 1996 and 2006 in the entire country, leading to 34–64 hospitalizations and 0–6 deaths per year, for an average fatality rate of 6.8%.[41] Of the 23 incidents recorded within Tokyo between 1993 and 2006, only one took place in a restaurant, while the others all involved fishermen eating their catch.[41] From 2006 through 2009 in Japan there were 119 incidents involving 183 people but only 7 people died.[42]

Only a few cases have been reported in the United States, and outbreaks in countries outside the Indo-Pacific area are rare. In Haiti, tetrodotoxin is thought to have been used in voodoo preparations, in so-called zombie poisons, where subsequent careful analysis has repeatedly called early studies into question on technical grounds, and have failed to identify the toxin in any preparation,[43][44][45] such that discussion of the matter has all but disappeared from the primary literature since the early 1990s. Kao and Yasumoto concluded in the first of their papers in 1986 that "the widely circulated claim in the lay press to the effect that tetrodotoxin is the causal agent in the initial zombification process is without factual foundation.”[43]:748

Genetic background is not a factor in susceptibility to tetrodotoxin poisoning. This toxicosis may be avoided by not consuming animal species known to contain tetrodotoxin, principally pufferfish; other tetrodotoxic species are not usually consumed by humans.

Fugu as a food

Poisoning from tetrodotoxin is of particular public health concern in Japan, where pufferfish "fugu" is a traditional delicacy. It is prepared and sold in special restaurants where trained and licensed chefs carefully remove the viscera to reduce the danger of poisoning.[46] There is potential for misidentification and mislabelling, particularly of prepared, frozen fish products.

Food analysis

The mouse bioassay developed for paralytic shellfish poisoning (PSP) can be used to monitor tetrodotoxin in pufferfish and is the current method of choice. An HPLC method with post-column reaction with alkali and fluorescence has been developed to determine tetrodotoxin and its associated toxins. The alkali degradation products can be confirmed as their trimethylsilyl derivatives by gas chromatography/mass spectrometry.

Detection in body fluids

Tetrodotoxin may be quantified in serum, whole blood or urine to confirm a diagnosis of poisoning in hospitalized patients or to assist in the forensic investigation of a case of fatal overdosage. Most analytical techniques involve mass spectrometric detection following gas or liquid chromatographic separation.[47]

Modern therapeutic research

Tetrodotoxin has been investigated as a possible treatment for cancer-associated pain. Early clinical trials demonstrate significant pain relief in some patients.[48][49]

In addition to the cancer pain application mentioned, mutations in one particular TTX-sensitive Na+ channel are associated with some migraine headaches,[50] although it is unclear as to whether this has any therapeutic relevance for most people with migraine.[51]

Tetrotoxin has been used clinically to relieve the headache associated with heroin withdrawal.[52]

Blocking of fast Na+ channels is already used to treat cardiac arrhythmias by a class of compounds called Class 1 antidysrythmic drugs; it is unclear as to whether using TTX to inhibit cardiac Na+ channels would help.


In the U.S., tetrodotoxin appears on the select agents list of the Department of Health and Human Services,[53] and scientists must register with HHS to use tetrodotoxin in their research. However, investigators possessing less than 100 mg are exempt from regulation.[54]

Popular culture

The effects of tetrodotoxin are used as a plot device in a number of movies and television series including:

  • Law Abiding Citizen (2009), when Shelton paralyzes Darby, without causing analgesia, in order to torture him more effectively.
  • Covert Affairs ("Starlings of the Slipstream," originally airing in November 2014) television series, causing the death of a fictional U.S. State Department official, leading to a fictional C.I.A. operation to identify and track the "rogue chemist" who synthesized the natural product on behalf of terrorists.[55][56]
  • Captain America: The Winter Soldier, causing the death of Nick Fury from Shield.
  • Nikita, to cause paralysis; in the show it has the ability to mask a person's vital signs from electronics, making that person appear dead.

Based on the presumption that tetrodotoxin is not always fatal, but at near-lethal doses can leave a person extremely unwell with the person remaining conscious,[35] tetrodotoxin has been alleged to result in zombieism, and has been suggested as an ingredient in Haitian Vodou preparations.[57] This idea appeared earlier, in the 1938 non-fiction book Tell My Horse by Zora Neale Hurston—reporting multiple accounts of purported tetrodotoxin poisoning in Haiti, by a voodoo sorcerer called the Bokor[58]—and popularized by Harvard-trained ethnobotanist Wade Davis,[57] but has been dismissed by the scientific community since the 1990s based on analytical chemistry-based tests of multiple preparations and review of earlier reports (see above).[43][44][45]

See also


  1. ^ Hogan CM (2008-12-02). "Rough-Skinned Newt Taricha granulosa". Retrieved 2009-04-06. 
  2. ^ Hwang DF, Tai KP, Chueh CH, Lin LC, Jeng SS (1991). "Tetrodotoxin and derivatives in several species of the gastropod Naticidae". Toxicon 29 (8): 1019–24.  
  3. ^ Lee CH, Ruben PC (2008). "Interaction between voltage-gated sodium channels and the neurotoxin, tetrodotoxin". Channels 2 (6): 407–12.  
  4. ^ Lewis AH, Raman IM (Nov 2014). "Resurgent current of voltage-gated Na(+) channels". The Journal of Physiology 592 (Pt 22): 4825–38.  
  5. ^ Narahashi T, Moore JW, Scott WR (May 1964). "Tetrodotoxin blockage of sodium conductance increase in lobster giant axons". The Journal of General Physiology 47: 965–74.  
  6. ^ Stokes, A. N.; Ducey, P. K.; Neuman-Lee, L.; Hanifin, C. T.; French, S. S.; Pfrender, M. E.; Brodie, E. D.; Brodie Jr., E. D. (2014). "Confirmation and Distribution of Tetrodotoxin for the First Time in Terrestrial Invertebrates: Two Terrestrial Flatworm Species (Bipalium adventitium and Bipalium kewense)". PLoS ONE 9 (6): e100718.  
  7. ^ a b Chau R, Kalaitzis JA, Neilan BA (Jul 2011). "On the origins and biosynthesis of tetrodotoxin". Aquatic Toxicology 104 (1-2): 61–72.  
  8. ^ Brodie ED, Brodie ED (May 1990). "Tetrodotoxin Resistance in Garter Snakes: An Evolutionary Response of Predators to Dangerous Prey". Evolution 44 (3): 651.  
  9. ^ Scheuer PJ. "Toxins from fish and other marine organisms". Advances in Food Research 18: 141–61.  
  10. ^ Trethewie ER (1978). "Tetrodotoxin in the blue-ringed octopus". Medical Journal of Australia 1 (9): 506. 
  11. ^ Hwang DF, Arakawa O, Saito T, Noguchi T, Simidu U, Tsukamoto K, Shida Y, Hashimoto K (1988). "Tetrodotoxin-producing bacteria from the blue-ringed octopus Octopus maculosus". Marine Biology 100 (3): 327–332.  
  12. ^ Noguchi T, Hwang DF, Arakawa O, Sugita H, Deguchi Y, Shida Y, Hashimoto K (1987). "Vibrio alginolyticus, a tetrodotoxin-producing bacterium, in the intestines of the fish Fugu vermicularis vermicularis" (PDF). Marine Biology 94 (4): 625–630.  
  13. ^ Thuesen EV Kogure K (1989). "Bacterial production of tetrodotoxin in four species of Chaetognatha" (PDF). Biological Bulletin 176 (2): 191–194.  
  14. ^ Carroll S, McEvoy EG, Gibson R (2003). "The production of tetrodotoxin-like substances by nemertean worms in conjunction with bacteria". Journal of experimental marine biology and ecology 288 (1): 51–63.  
  15. ^ Moczydlowski EG (Mar 2013). "The molecular mystique of tetrodotoxin". Toxicon 63: 165–83.  
  16. ^ "Tetrodotoxin". Guide to Pharmacology. IUPHAR/BPS. Retrieved 22 August 2015. 
  17. ^  
  18. ^ Kishi Y, Aratani M, Fukuyama T, Nakatsubo F, Goto T (Dec 1972). "Synthetic studies on tetrodotoxin and related compounds. 3. A stereospecific synthesis of an equivalent of acetylated tetrodamine". Journal of the American Chemical Society 94 (26): 9217–9.  
  19. ^ Kishi Y, Fukuyama T, Aratani M, Nakatsubo F, Goto T (Dec 1972). "Synthetic studies on tetrodotoxin and related compounds. IV. Stereospecific total syntheses of DL-tetrodotoxin". Journal of the American Chemical Society 94 (26): 9219–21.  
  20. ^ Ohyabu N, Nishikawa T, Isobe M (Jul 2003). "First asymmetric total synthesis of tetrodotoxin". Journal of the American Chemical Society 125 (29): 8798–805.  
  21. ^ Nishikawa T, Urabe D, Isobe M (Sep 2004). "An efficient total synthesis of optically active tetrodotoxin". Angewandte Chemie 43 (36): 4782–5.  
  22. ^ Taber D (2005-05-02). "Synthesis of (-)-Tetrodotoxin". Organic Chemistry Portal. Retrieved 2008-05-29. 
  23. ^ Hinman A, Du Bois J (Sep 2003). "A stereoselective synthesis of (-)-tetrodotoxin". Journal of the American Chemical Society 125 (38): 11510–1.  
  24. ^ Sato K, Akai S, Yoshimura J (Jul 2013). "Stereocontrolled total synthesis of tetrodotoxin from myo-inositol and D-glucose by three routes: aspects for constructing complex multi-functionalized cyclitols with branched-chain structures". Natural Product Communications 8 (7): 987–98.  
  25. ^ Chau J, Ciufolini MA (2011). "The chemical synthesis of tetrodoxin: an ongoing quest". Marine Drugs 9 (10): 2046–74.  
  26. ^ "Material Safety Data Sheet Tetrodotoxin ACC# 01139". Acros Organics N.V. 
  27. ^ "Cyanides (as CN)". Immediately Dangerous to Life and Health.  
  28. ^ Gilman AG, Goodman LS, Gilman AZ (1980). Goodman & Gilman's The pharmacological Basis of Therapeutics. New York: McGraw-Hill. p. 310.  
  29. ^ Patockaa J, Stredab L (April 23, 2002). Price R, ed. "Brief Review of Natural Nonprotein Neurotoxins". ASA Newsletter (Applied Science and Analysis inc.) 02–2 (89): 16–23.  
  30. ^ a b c d e f Clark RF, Williams SR, Nordt SP, Manoguerra AS (1999). "A review of selected seafood poisonings". Undersea & Hyperbaric Medicine 26 (3): 175–84.  
  31. ^ Bane V, Lehane M, Dikshit M, O'Riordan A, Furey A (Feb 2014). "Tetrodotoxin: chemistry, toxicity, source, distribution and detection". Toxins 6 (2): 693–755.  
  32. ^ Rang H, Ritter J, Flower R, Henderson G (2015). Rang & Dale's Pharmacology (8th ed.). Churchill Livingstone.  
  33. ^ a b c Kao CY (Jun 1966). "Tetrodotoxin, saxitoxin and their significance in the study of excitation phenomena". Pharmacological Reviews 18 (2): 997–1049.  
  34. ^ "T8024 Sigma Tetrodotoxin". Catalogue. Sigma-Aldrich. Retrieved 23 August 2015. 
  35. ^ a b c d Butterton JR, Calderwell SB (1998). "Acute infectious diarrhoea disease and bacterial food poisoning". In Fauci AS, Braunwald E, Isselbacher KJ, Wilson JD, Martin JB, Kasper DL, Hauser SL, Longo DL. Harrison's principles of internal medicine (14th ed.). New York: McGraw-Hill, Health Professions Division. pp. 796–601.  
  36. ^ a b Benzer T. "Tetrodotoxin Toxicity". Medscape. Retrieved 23 August 2015. 
  37. ^ Rivera VR, Poli MA, Bignami GS (Sep 1995). "Prophylaxis and treatment with a monoclonal antibody of tetrodotoxin poisoning in mice". Toxicon 33 (9): 1231–7.  
  38. ^ Bradley SG, Klika LJ (Jul 1981). "A fatal poisoning from the Oregon rough-skinned newt (Taricha granulosa)". Jama 246 (3): 247.  
  39. ^ McNabb P, Mackenzie L, Selwood A, Rhodes L, Taylor D, Cornelison C (2009). and coincidence of dog deaths along Auckland Beaches."Pleurobranchaea maculata"Review of tetrodotoxins in the sea slug (PDF). Auckland Regional Council Technical Report 2009/108. Cawthron Institute for the Auckland Regional Council. 
  40. ^ Gibson E (15 August 2009). "Puffer fish toxin blamed for deaths of two dogs".  
  41. ^ a b 危険がいっぱい ふぐの素人料理 [Danger in fugu amateur cuisine] (in Japanese). Tokyo Bureau of Social Welfare and Public Health. Archived from the original on 28 January 2010. 
  42. ^ 自然毒のリスクプロファイル:魚類:フグ毒 [Fish: fugu poison risk profile of natural poison] (in Japanese). 厚生労働省 (Ministry of Health Labour and Welfare (Japan)). Archived from the original on 27 September 2011. 
  43. ^ a b c Yasumoto T, Kao CY. "Tetrodotoxin and the Haitian zombie". Toxicon 24 (8): 747–9.  
  44. ^ a b Kao CY, Yasumoto T. "Tetrodotoxin in "zombie powder"". Toxicon 28 (2): 129–32.  
  45. ^ a b Hines T (May–June 2008). "Zombies and Tetrodotoxin". Skeptical Inquirer 32.3: 60–62. 
  46. ^ Warin, Rosemary H.; Steventon, Glyn B.; Mitchell, Steve C. (2007). Molecules of death. Imperial College Press. p. 390.  
  47. ^ Baselt RC (2008). Disposition of toxic drugs and chemicals in man (8th ed.). Foster City, California: Biomedical Publications. pp. 1521–22.  
  48. ^ Hagen NA, Lapointe B, Ong-Lam M, Dubuc B, Walde D, Gagnon B, Love R, Goel R, Hawley P, Ngoc AH, du Souich P (Jun 2011). "A multicentre open-label safety and efficacy study of tetrodotoxin for cancer pain". Current Oncology 18 (3): e109–16.  
  49. ^ Hagen NA, du Souich P, Lapointe B, Ong-Lam M, Dubuc B, Walde D, Love R, Ngoc AH (Apr 2008). "Tetrodotoxin for moderate to severe cancer pain: a randomized, double blind, parallel design multicenter study". Journal of Pain and Symptom Management 35 (4): 420–9.  
  50. ^ Nieto FR, Cobos EJ, Tejada MÁ, Sánchez-Fernández C, González-Cano R, Cendán CM (Feb 2012). "Tetrodotoxin (TTX) as a therapeutic agent for pain". Marine Drugs 10 (2): 281–305.  
  51. ^ Stimmel B (2002). "12: Heroin Addiction". Alcoholism, drug addiction, and the road to recovery: life on the edge. New York: Haworth Medical Press.  
  52. ^ Song H, Li J, Lu CL, Kang L, Xie L, Zhang YY, Zhou XB, Zhong S (Aug 2011). "Tetrodotoxin alleviates acute heroin withdrawal syndrome: a multicentre, randomized, double-blind, placebo-controlled study". Clinical and Experimental Pharmacology & Physiology 38 (8): 510–4.  
  53. ^ "HHS and USDA Select Agents and Toxins 7 CFR Part 331, 9 CFR Part 121, and 42 CFR Part 73." (PDF). Archived from the original (PDF) on 17 January 2009. Retrieved 17 March 2013. 
  54. ^ "Permissible Toxin Amounts". Federal Select Agent Program. United States Centers for Disease Control and Prevention. Retrieved 17 March 2013. 
  55. ^ Miranda K (26 November 2014). "Covert Affairs Recap: Starlings of the Slipstream". Movie News Guide. Retrieved 25 July 2015. 
  56. ^ "Covert Affairs: Starlings of the Slipstream (season 5, episode 12 , original air date 13 November 2014)". USA Networks. 2015. Retrieved 25 July 2015. 
  57. ^ a b Davis W (1985). ' 
  58. ^ Hurston ZN (2009). Reed I, Louis H, eds. Tell my horse: Voodoo and life in Haiti and Jamaica (1st Harper Perennial Modern Classics ed.). New York: Harper Perennial. p. 336.  

External links

  • Tetrodotoxin at the US National Library of Medicine Medical Subject Headings (MeSH)
  • Tetrodotoxin: essential data (1999)
  • Tetrodotoxin from the Bad Bug Book at the U.S. Food and Drug Administration website
  • New York Times, "Whatever Doesn't Kill Some Animals Can Make Them Deadly"
  • U.S. National Library of Medicine: Hazardous Substances Databank – Tetrodotoxin
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