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Anatoxins
The basic mechanism of muscle
contraction consists of the neurotransmitter acetylcholine
propagating from the axon of a nerve cell to the ion channels in the
wall of a muscle cell. The acetylcholine binds to the ion channel,
opening it and allowing the migration of ions across the muscle cell
wall, thus propagating the electrical signal for the cell to
contract. It is then the job of the enzyme cholinesterase to
deactivate the cholinesterase and allow the ion channel to re-close,
relaxing the contraction.
Anatoxin-a is an alkaloid that acts as an
acetylcholine mimic, and is thus able to bind to and open the ion
channel. It cannot, however, be deactivated acetylcholinesterase,
and so the ion channel stays open. The muscle cell continues to
contract until it fails from exhaustion.
Anatoxin-a(s), the second
type of anatoxin, only occurs in the species Anabaena flos-aquae,
one of the most toxic strains of cyanobacteria. It is an
acetylcholinesterase inhibitor which binds to the enzyme and renders
it unable to deactivate the acetylcholine. Since the acetylcholine
is not deactivated, the ion channel is left open, once again
destroying muscle function through exhaustion. Anatoxin-a(s) is an
organic phosphate, similar in its action to synthetic
organophosphate pesticides such as parathion and malathion.
Anatoxin-a(s) is the only natural organophosphate known. Since it is
more water soluble than synthetic organophosphates, with
consequently less tendency to bioaccumulate and stay in fat cells
and cell membranes, it may yield a less nefarious pesticide than its
synthetic brethren.
Anatoxins
The anatoxins are a group of low
molecular weight neurotoxic alkaloids first described in the
fresh-water cyanobacteria Anabaena flos-aquae from Canada (Gorham
et
al., 1964). Anatoxins have not yet been identified in Australian
cyanobacteria. three common anatoxins have been described: anatoxin-a
and homoanatoxin-a are secondary amines and anatoxin-a(S) is a
phosphate ester of a cyclic N-hydroxyguanine structure (Figure 1).
Figure
1: Anatoxin
Further Reading
Toxic Cyanobacteria in Water: a guide
to their public health consequences, monitoring and management.
Chorus, E. & Bartram, J. (Eds.) World Health Organisation 1999,
E&FN Spoon London & New York.
Reference
Gorham
PJ, McLachlan
J, Hammer UT & Kim, W.K. (1964) Isolation and toxic strains of
Anabaena flos-aquae (lyngb.) de Breb. Verh. Internat. Verein.
Limnol. XV, 796-804
Anatoxin production
The
anatoxins have been identified in freshwater cyanobacteria from
Europe, North America and Japan (see Table 1) but have not been
identified in Australian cyanobacteria. Anatoxins are produced by
various species of cyanobacteria, in isolation or in combination
with hepatotoxins (Fig. 1). Not all strains of the causative species
are toxic and there are no taxonomical or behavioural clues to the
presence or absence of anatoxin in a particular sample.
Table
1. Sources of anatoxins
worldwide*
| Toxin |
Cyanobacteria |
Country |
|
Anatoxin-a |
Anabaena
flos-aquae |
Canada,
Finland |
|
|
Anabaena
planktonia |
Italy |
|
|
Oscillatoria |
Scotland,
Ireland |
|
|
Aphanizomenon |
Germany,
Finland |
|
|
Cylindrospermum |
Finland |
|
|
Microsystis |
Japan |
|
|
|
|
Homoanatoxin-a |
Oscillatoria
formosa |
Norway |
|
|
|
|
Anatoxin-a(S) |
Anabaena
flos-aquae |
Canada,
Denmark |
|
|
Anabaena
lemmermannii |
Denmark |
*Adapted from Toxic Cyanobacteria in
Water: a guide to their public health consequences, monitoring and
management. Chorus, E. & Bartram, J. (Eds.) World Health
Organisation 1999, E&FN Spoon London & New York.
Anatoxin poisoning
Anatoxin-a
and homoanatoxin-a are postsynaptic depolarising neuromuscular
blocking agents (Carmichael et al. 1979) that bind strongly
to the nicotinic acetylcholine receptor (Spivak et al.,
1980). These compounds are potent neurotoxins which cause rapid
death in mammals by respiratory arrest (mouse LD50 approx
250 m g/kg IP, Devlin et al., 1977).
Anatoxin-a(S)
is more potent towards mice (LD50 20-50 m g/kg) and is a
cholinesterase inhibitor (Mahmood & Carmichael, 1986;1987).
Unlike anatoxin-a, anatoxin-a(S) induces hypersalivation in mammals
as well as other symptoms more typical of neurotoxicity such as
diarrhoea, shaking and nasal mucus discharge (Cook et al.,
1991).
Detailed
reading
Carmichael WW, Biggs, DF, & Gorham PR (1977). Toxicology and
pharmacological action of Anabaena flos-aquae toxin. Science
187, 542-544.
Cook WO, Beasley VR, Lovell RA, Dahlem AM, Hooser SB, Mahmood, NA
& Carmichale WW (1989) Consistent inhibition of peripheral
cholinesterases by neurotoxins from the freshwater cyanobacterium Anabaena
flos-aquae: Studies of ducks, swine, mice and a steer. Environ.
Toxicol. Chem 8, 915-922.
Devlin JP, Edwards OE, Gorham PR, Hunter NR, Pike RK &
Starvick B (1977) Anatoxin-a, a toxic alkaloid from Anabaena flos-aquae
NCR-44h. Can. J. Chem. 55, 1367-1371.
Mahmood NA & Carmichael WW (1986) The pharmacology of
anatoxin-a(s), a neurotoxin produced by the freshwater
cyanobacterium Anabaena flos-aquae NRC 525-17. Toxicon 24, 425-434.
Mahmood NA & Carmichael WW (1987) Anatoxin-a(s), an
anticholinesterase from the cyanobacterium Anabaena flos-aquae NRC
525-17. Toxicon 25, 1221-1227.
Spivak CE, Witkop, B & Albuquerque, EX (1980) Anatoxin-a: a
novel, potent agonist at the nicotinic receptor. Mol. Pharmacol. 18,
384-394.
e-mail: web@aims.gov.au
Page last updated -
December 18, 2008
©2000-2005 Australian Research Network for Algal Toxins
URL http://www.aims.gov.au/arnat
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