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首页> 外文期刊>Journal of Insect Physiology >Mechanisms of transport of H+, Na+ and K+, across the distal gastric caecum of larval Aedes aegypti
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Mechanisms of transport of H+, Na+ and K+, across the distal gastric caecum of larval Aedes aegypti

机译:H +,Na +和k +的运输机制,幼虫AEDES AEGYPTI的远端胃部

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摘要

Measured changes in ion fluxes, transepithelial potential (TEP) and basolateral membrane potential (V-b) in response to ion transporter inhibitors were used to assess the mechanisms of transport of H+, Na+ and K+, across the distal gastric caecum of larval Aedes aegypti, a vector of yellow fever. Preparations were stimulated with 5-hydroxytryptamine (5-HT, 10(-6) M) in order to maintain stable rates of H+, Na+, and K+ transport across the distal caecum. Transepithelial potential (TEP), basolateral membrane potential (Vb), and H+, Na+ and K+ fluxes all declined after the addition of a vacuolar-type H+-ATPase (VA) inhibitor, n-ethlymaleimide (NEM), consistent with a primary role for VA in energizing ion transport across the distal gastric caecum. Amiloride also inhibited H+, Na+, and K+ fluxes, consistent with an apically expressed VA that is coupled to a cation:H+ antiporter (AeNHE8), analogous to the coupling of apical VA and cation:nH(+) antiporter in Malpighian tubules. A working model of transport of H+, Na+ and K+ across the distal gastric caecum proposes that coupling of VA and AeNHE8 in the apical membrane leads to the removal of intracellular Na+ or K+, thus creating favourable ion gradients to promote the activity of two transporters in the basal membrane, cation:H+ antiporter (AeNHE3) and a bumetanide-sensitive cation chloride cotransporter (CCC).
机译:用于响应离子转运蛋白抑制剂的离子通量,Transephelial电位(TEP)和基石运动膜电位(VB)的测量变化用于评估H +,Na +和K +的运输机制,在幼虫AEDESAEGYPTI,A黄热病传染媒介。用5-羟基三胺(5-HT,10(-6)M)刺激制剂,以保持在远端凹凸上的H +,Na +和K +运输的稳定速率。在添加真空型H + -ATP酶(VA)抑制剂,N-乙基酰亚胺(NEM)后,Transepithelial电位(Tep),基石膜电位(VB)和H +,Na +和K +倍倍次均下降用于VA在远端胃毛窦上激励离子输送。氨基甲胺还抑制了H +,Na +和K +助熔剂,与顶表达的VA一致,其偶联至阳离子:H +炔菌剂(AENHE8),类似于顶端VA和阳离子的偶联:Malpighian小管中的NH(+)抗糖剂。远端胃咬伤的H +,Na +和K +的运输模型提出了VA和AENHE8在顶端膜中的偶联导致细胞内Na +或K +的去除,从而产生有利的离子梯度,以促进两个转运镜的活性基础膜,阳离子:H +抗抗原剂(AENHE3)和胆敏敏感阳离子氯化物分类剂(CCC)。

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