1997
DOI: 10.1016/s0079-6603(08)61036-3
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Molecular Evolution of Snake Toxins: Is the Functional Diversify of Snake Toxins Associated with a Mechanism of Accelerated Evolution?

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Cited by 195 publications
(131 citation statements)
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“…Thus, except for these proteins, all of which were found in the pooled venoms (Table 2), the peptide mass fingerprinting approach alone was unable to identify any protein in the databases. In addition, as expected from the rapid amino acid sequence divergence of venom proteins evolving under accelerated evolution, [50][51][52][53][54][55][56] with a few exceptions, the product ion spectra did not match any known protein. Hence, mass spectra were manually interpreted for de novo sequencing and the CID-MS/ MS-deduced peptide ion sequences (Table 2) were submitted to BLAST similarity searches.…”
Section: Results and Discusionmentioning
confidence: 99%
“…Thus, except for these proteins, all of which were found in the pooled venoms (Table 2), the peptide mass fingerprinting approach alone was unable to identify any protein in the databases. In addition, as expected from the rapid amino acid sequence divergence of venom proteins evolving under accelerated evolution, [50][51][52][53][54][55][56] with a few exceptions, the product ion spectra did not match any known protein. Hence, mass spectra were manually interpreted for de novo sequencing and the CID-MS/ MS-deduced peptide ion sequences (Table 2) were submitted to BLAST similarity searches.…”
Section: Results and Discusionmentioning
confidence: 99%
“…Polymorphic PLA 2 genes and mRNAs are usually found in snake venom glands [25]. Six of the 10 C. rhodostoma PLA 2 clones are apparently not translated into venom proteins.…”
Section: Untranslated Pla 2 Mrnasmentioning
confidence: 99%
“…Peptide toxins from venomous creatures have served as vital tools to define the molecular mechanisms underlying K ϩ channel function (1,2). It has been suggested that toxins evolved from endogenous genes that function in normal cellular pathways (3,4). Indeed, venomous creatures possess toxins with homology to several proteins, including acetylcholinesterases (5), phospholipases (6,7), nerve growth factor (8), endothelins (9), Lynx-1 (10,11), Kunitz-type serine protease inhibitors (12), and the ion channel regulatory (ICR) 5 domains of cysteinerich secretory proteins (CRISPs) (3,13,14).…”
mentioning
confidence: 99%