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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Characterisation of penicillin-G uptake in rabbit small-intestinal brush-border membrane vesicles
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Characterisation of penicillin-G uptake in rabbit small-intestinal brush-border membrane vesicles

机译:兔小肠刷状边界膜囊泡中青霉素-G摄取的特征

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摘要

Uptake of penicillin-G has been studied in rabbit intestinal brush-border membrane vesicles (BBMV). Penicillin-G was transported into the lumen of BBMV via an H+-dependent, Na+-independent uptake system. This was a saturable carrier-mediated process, which adhered to Michaelis-Menten kinetics, having a pH optimum of 4.5 and resulting in a net-negative charge transfer. Vmax was 59 nmol penicillin-G (mg protein)-1 (30 s)-1 and Km 22.7 mM. Ampicillin, penicillin-V, cefadroxil, cephalexin, cephalothin, cephradine, -camosine, glycyl--alanine, glycyl--tyrosine and glycylglycylglycine inhibited the uptake of penicillin-G. However, glycylsarcosine stimulated uptake by 92%. Countertransport experiments suggested that this effect took place at the active site of the transporter. Penicillin-G uptake appeared to be mediated via a common transport system shared by penicillins, cephalosporins and peptides.
机译:已经在兔肠刷状边界膜囊泡(BBMV)中研究了青霉素-G的吸收。青霉素-G通过依赖H +,不依赖Na +的吸收系统转运到BBMV腔中。这是一个可饱和的载体介导的过程,该过程遵循Michaelis-Menten动力学,最适pH为4.5,导致净负电荷转移。 Vmax为59 nmol青霉素-G(mg蛋白)-1(30 s)-1和Km 22.7 mM。氨苄青霉素,青霉素-V,头孢羟氨苄,头孢氨苄,头孢菌素,头孢拉定,-肌氨酸,甘氨酰-丙氨酸,甘氨酰-酪氨酸和甘氨酰甘氨酰甘氨酸抑制青霉素-G的摄取。然而,甘氨酸肌氨酸刺激摄取92%。反转运实验表明,这种效应发生在转运蛋白的活性位点。青霉素-G的摄取似乎是由青霉素,头孢菌素和肽共有的共同转运系统介导的。

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