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Influence of codon usage bias on FGLamide-allatostatin mRNA secondary structure.

机译:密码子使用偏倚对FGLamide-阿拉托他汀mRNA二级结构的影响。

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The FGLamide allatostatins (ASTs) are invertebrate neuropeptides which inhibit juvenile hormone biosynthesis in Dictyoptera and related orders. They also show myomodulatory activity. FGLamide AST nucleotide frequencies and codon bias were investigated with respect to possible effects on mRNA secondary structure. 367 putative FGLamide ASTs and their potential endoproteolytic cleavage sites were identified from 40 species of crustaceans, chelicerates and insects. Among these, 55% comprised only 11 amino acids. An FGLamide AST consensus was identified to be (X)(1-->16)Y(S/A/N/G)FGLGKR, with a strong bias for the codons UUU encoding for Phe and AAA for Lys, which can form strong Watson-Crick pairing in all peptides analyzed. The physical distance between these codons favor a loop structure from Ser/Ala-Phe to Lys-Arg. Other loop and hairpin loops were also inferred from the codon frequencies in the N-terminal motif, and the first amino acids from the C-terminal motif, or the dibasic potential endoproteolytic cleavage site. Our results indicate that nucleotide frequencies and codon usage bias in FGLamide ASTs tend to favor mRNA folds in the codon sequence in the C-terminal active peptide core and at the dibasic potential endoproteolytic cleavage site.
机译:FGLamide allatostatins(ASTs)是无脊椎动物神经肽,可抑制双翅目和相关命令中幼体激素的生物合成。它们还显示出肌调节活性。关于对mRNA二级结构的可能影响,研究了FGLamide AST核苷酸频率和密码子偏倚。从40种甲壳类动物,螯合物和昆虫中鉴定出367种推定的FGLamide AST及其潜在的内切蛋白裂解位点。其中55%仅包含11个氨基酸。 FGLamide AST共识被确定为(X)(1-> 16)Y(S / A / N / G)FGLGKR,对Phe的密码子UUU和Lys的AAA具有强烈的偏见,可以形成所有分析的肽中的沃森-克里克配对。这些密码子之间的物理距离有利于从Ser / Ala-Phe到Lys-Arg的环状结构。还可以从N端基序中的密码子频率以及C端基序中的第一个氨基酸或二元潜在内切蛋白水解位点推断出其他环和发夹环。我们的结果表明,FGLamide AST中的核苷酸频率和密码子使用偏向倾向于在C末端活性肽核心和二元潜在内切蛋白水解位点的密码子序列中促进mRNA折叠。

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