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Genomic and Structural Characterization of Kunitz-Type Peptide LmKTT-1a Highlights Diversity and Evolution of Scorpion Potassium Channel Toxins. e60201
by
Chen, Zongyun
, Yang, Weishan
, Liu, Maili
, Feng, Jing
, Cao, Zhijian
, Zeng, Danyun
, Li, Wenxin
, Jiang, Ling
, Luo, Fan
, Zhao, Ruiming
in
Channelopathy
2013
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Genomic and Structural Characterization of Kunitz-Type Peptide LmKTT-1a Highlights Diversity and Evolution of Scorpion Potassium Channel Toxins. e60201
by
Chen, Zongyun
, Yang, Weishan
, Liu, Maili
, Feng, Jing
, Cao, Zhijian
, Zeng, Danyun
, Li, Wenxin
, Jiang, Ling
, Luo, Fan
, Zhao, Ruiming
in
Channelopathy
2013
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Genomic and Structural Characterization of Kunitz-Type Peptide LmKTT-1a Highlights Diversity and Evolution of Scorpion Potassium Channel Toxins. e60201
by
Chen, Zongyun
, Yang, Weishan
, Liu, Maili
, Feng, Jing
, Cao, Zhijian
, Zeng, Danyun
, Li, Wenxin
, Jiang, Ling
, Luo, Fan
, Zhao, Ruiming
in
Channelopathy
2013
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Genomic and Structural Characterization of Kunitz-Type Peptide LmKTT-1a Highlights Diversity and Evolution of Scorpion Potassium Channel Toxins. e60201
Journal Article
Genomic and Structural Characterization of Kunitz-Type Peptide LmKTT-1a Highlights Diversity and Evolution of Scorpion Potassium Channel Toxins. e60201
2013
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Overview
Background Recently, a new subfamily of long-chain toxins with a Kunitz-type fold was found in scorpion venom glands. Functionally, these toxins inhibit protease activity and block potassium channels. However, the genomic organization and three-dimensional (3-D) structure of this kind of scorpion toxin has not been reported. Principal Findings Here, we characterized the genomic organization and 3-D nuclear magnetic resonance structure of the scorpion Kunitz-type toxin, LmKTT-1a, which has a unique cysteine pattern. The LmKTT-1a gene contained three exons, which were interrupted by two introns located in the mature peptide region. Despite little similarity to other Kunitz-type toxins and a unique pattern of disulfide bridges, LmKTT-1a possessed a conserved Kunitz-type structural fold with one alpha -helix and two beta -sheets. Comparison of the genomic organization, 3-D structure, and functional data of known toxins from the alpha -KTx, beta -KTx, gamma -KTx, and Kappa -KTx subfamily suggested that scorpion Kunitz-type potassium channel toxins might have evolved from a new ancestor that is completely different from the common ancestor of scorpion toxins with a CS alpha / beta fold. Thus, these analyses provide evidence of a new scorpion potassium channel toxin subfamily, which we have named delta -KTx. Conclusions/Significance Our results highlight the genomic, structural, and evolutionary diversity of scorpion potassium channel toxins. These findings may accelerate the design and development of diagnostic and therapeutic peptide agents for human potassium channelopathies.
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