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Functional Hypervariability and Gene Diversity of Cardioactive Neuropeptides

机译:心脏活性神经肽的功能性高变性和基因多样性

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Crustacean cardioactive peptide (CCAP) and related peptides are multifunctional regulatory neurohormones found in invertebrates. We isolated a CCAP-related peptide (conoCAP-a, for cone snail CardioActive Peptide) and cloned the cDNA of its precursor from venom of Conus villepinii. The precursor of conoCAP-a encodes for two additional CCAP-like peptides: conoCAP-b and conoCAP-c. This multi-peptide precursor organization is analogous to recently predicted molluscan CCAP-like preprohormones, and suggests a mechanism for the generation of biological diversification without gene amplification. While arthropod CCAP is a cardio-accelerator, we found that conoCAP-a decreases the heart frequency in Drosophila larvae, demonstrating that conoCAP-a and CCAP have opposite effects. Intravenous injection of conoCAP-a in rats caused decreased heart frequency and blood pressure in contrast to the injection of CCAP, which did not elicit any cardiac effect. Perfusion of rat ventricular cardiac myocytes with conoCAP-a decreased systolic calcium, indicating that conoCAP-a cardiac negative inotropic effects might be mediated via impairment of intracellular calcium trafficking. The contrasting cardiac effects of conoCAP-a and CCAP indicate that molluscan CCAP-like peptides have functions that differ from those of their arthropod counterparts. Molluscan CCAP-like peptides sequences, while homologous, differ between taxa and have unique sequences within a species. This relates to the functional hypervariability of these peptides as structure activity relationship studies demonstrate that single amino acids variations strongly affect cardiac activity. The discovery of conoCAPs in cone snail venom emphasizes the significance of their gene plasticity to have mutations as an adaptive evolution in terms of structure, cellular site of expression, and physiological functions.
机译:甲壳类贲门活性肽(CCAP)和相关肽是无脊椎动物中发现的多功能调节神经激素。我们分离CCAP相关的肽(COOOCAP-A,用于锥形蜗牛心脏肿瘤致癌肽),并将其前体的cDNA克隆来自康斯·韦尔斯顿菌的毒液。 COOCAP-A类似CCAP样肽的编码前体:COOCAP-B和COOCAP-C.这种多肽前体组织类似于最近预测的软体动物CCAP样预肢体,并提出了在没有基因扩增的情况下产生生物多样化的机制。虽然节肢动物CCAP是一种有氧运动,但我们发现Conocap-A降低了果蝇幼虫中的心脏频率,展示了COOCAP-A和CCAP具有相反的效果。静脉内注射大鼠的COOCAP-A引起的心脏频率和血压与注射CCAP相比,这并未引发任何心脏效应。用CONOCAP-A减少的收缩钙灌注大鼠心室心肌细胞,表明CONOCAP-A心脏阴性渗透效应可能通过细胞内钙贩运的损害来介导。 COOCAP-A和CCAP的对比心脏作用表明软体动物CCAP样肽具有与其节肢动物对应物不同的功能。软体动物CCAP肽序列,同时同源,分类率不同,并且在物种中具有独特的序列。这涉及这些肽的功能性高价值,因为结构活动关系研究表明单一氨基酸变化强烈影响心脏活性。锥形蜗牛毒液的发现强调了它们基因可塑性在结构,表达细胞部位和生理功能方面具有突变作为自适应演变的重要性。

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