首页> 外文期刊>The Journal of Membrane Biology >Lysine Uptake by Cloned hCAT-2B: Comparison with hCAT-1 and with Trophoblast Surface Membranes
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Lysine Uptake by Cloned hCAT-2B: Comparison with hCAT-1 and with Trophoblast Surface Membranes

机译:克隆的hCAT-2B对赖氨酸的吸收:与hCAT-1和滋养层表面膜的比较

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摘要

To study the cationic amino-acid transporter hCAT-2B of human placenta, total RNA was harvested from primary cultured trophoblast and from the BeWo choriocarcinoma cell line (b30 clone) and used for reverse transcription (RT) and polymerase chain reaction (PCR). Primers based on published sequences identified expression of mRNA for hCAT-2B. RT-PCR yielded a 2.06 kb hCAT-2B cDNA, which was cloned. hCAT-2B cRNA injection into Xenopus laevis oocytes stimulated saturable lysine uptake (Km ~ 125 mM). In the presence of Na+, uptake was completely inhibited by L-arginine but only partially by neutral amino acids. To compare directly the interaction of hCAT-1 and hCAT-2B with neutral amino acids and sodium, we examined the inhibition of these transporters by L-leucine and L-alanine over a wide concentration range. L-Alanine and L-leucine inhibit uptake by hCAT-2B substantially less completely than uptake by hCAT-1. The interaction of hCAT-2B resembles that of system y+ in the microvillous membrane of human placenta, while that of hCAT-1 is more comparable to that of system y+ in basal membrane. The identification and characterization of the various cationic amino-acid transporters of the human placenta have the potential to increase the understanding of the cellular mechanism of transplacental transfer.
机译:为了研究人类胎盘的阳离子氨基酸转运蛋白hCAT-2B,从原代培养的滋养细胞和BeWo绒毛膜癌细胞株(b30克隆)中收获总RNA,并将其用于逆转录(RT)和聚合酶链反应(PCR)。基于公开序列的引物鉴定了hCAT-2B的mRNA表达。 RT-PCR产生2.06 kb hCAT-2B cDNA,将其克隆。将hCAT-2B cRNA注射到非洲爪蟾卵母细胞中可刺激饱和赖氨酸摄取(Km〜125 mM)。在Na +存在下,L-精氨酸会完全抑制摄取,但中性氨基酸只会部分抑制摄取。为了直接比较hCAT-1和hCAT-2B与中性氨基酸和钠的相互作用,我们研究了L-亮氨酸和L-丙氨酸在很宽的浓度范围内对这些转运蛋白的抑制作用。 L-丙氨酸和L-亮氨酸抑制hCAT-2B的吸收要比抑制hCAT-1的吸收少得多。 hCAT-2B的相互作用类似于人胎盘微绒膜中系统y +的相互作用,而hCAT-1的相互作用与基膜中系统y +的相互作用更相似。人胎盘的各种阳离子氨基酸转运蛋白的鉴定和表征具有增加对跨胎盘转运的细胞机制的理解的潜力。

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  • 来源
    《The Journal of Membrane Biology》 |2002年第1期|27-33|共7页
  • 作者单位

    Department of Pediatrics Box 8116 Washington University School of Medicine at St. Louis Children's Hospital One Children's Place St. Louis MO 63110 USA;

    Department of Pediatrics Box 8116 Washington University School of Medicine at St. Louis Children's Hospital One Children's Place St. Louis MO 63110 USA;

    Department of Pediatrics Box 8116 Washington University School of Medicine at St. Louis Children's Hospital One Children's Place St. Louis MO 63110 USA;

    Department of Pediatrics Box 8116 Washington University School of Medicine at St. Louis Children's Hospital One Children's Place St. Louis MO 63110 USA;

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  • 入库时间 2022-08-18 01:42:19

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