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尿毒症血清残留物通过抑制 LS-180 结肠癌细胞中的有机阴离子转运多肽 2B1 降低 SN-38 的敏感性。

Uremic serum residue decreases SN-38 sensitivity through suppression of organic anion transporter polypeptide 2B1 in LS-180 colon cancer cells.

机构信息

Department of Clinical Pharmacy, Faculty of Pharmaceutical Science, Kyoto Pharmaceutical University, 5 Misasagi Nakauchi-cho, Yamashina-ku, Kyoto, 607-8414, Japan.

Scientific Research and Business Development Department, Towa Pharmaceutical Co. Ltd., Kyoto Research Park KISTIC#202, 134 Chudoji Minami-Machi, Shimogyo-ku, Kyoto, 600-8813, Japan.

出版信息

Sci Rep. 2019 Oct 29;9(1):15464. doi: 10.1038/s41598-019-51640-9.

DOI:10.1038/s41598-019-51640-9
PMID:31664047
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6820778/
Abstract

Pharmacokinetics of SN-38 in patients with end-stage kidney disease (ESKD) is partially varied because of fluctuations in transporters expression and/or function by high protein bound-uremic toxins concentration. The fluctuations may induce variations in anticancer drugs sensitivity to cancer cells. We aimed to clarify the variations in sensitivity of SN-38 to cancer patients with ESKD and investigate this mechanism, by human colon cancer cells exposed to uremic serum residue. LS180 cells were exposed to normal or uremic serum residue (LS/NSR or LS/USR cells) for a month. IC values of SN-38 in LS/NSR or LS/USR cells were calculated from viability of each cells treated SN-38. mRNA expression and intracellular SN-38 accumulation was evaluated by RT-PCR and HPLC-fluorescence methods, respectively. The IC value in LS/USR cells was higher than that in LS/NSR cells. Organic anion transporter polypeptide (OATP) 2B1 mRNA expression was lower in LS/USR cells than in LS/NSR cells, and SN-38 accumulation in LS/USR cells was lower than that in LS/NSR cells. Only co-treatment baicalin, which is OATP2B1 inhibitor, almost negated the difference in SN-38 accumulation between LS/NSR and LS/USR. Anticancer effects of substrates of OATP2B1, such as SN-38, were reduced in ESKD patients at the same plasma substrate concentration.

摘要

终末期肾病(ESKD)患者的 SN-38 药代动力学部分因高蛋白结合尿毒症毒素浓度导致转运体表达和/或功能波动而发生变化。这种波动可能会导致抗癌药物对癌细胞的敏感性发生变化。我们旨在通过人结肠癌细胞暴露于尿毒症血清残余物来阐明 ESKD 癌症患者对 SN-38 敏感性的变化,并研究这种机制。LS180 细胞在正常或尿毒症血清残余物(LS/NSR 或 LS/USR 细胞)中暴露一个月。从用 SN-38 处理的每种细胞的活力计算 SN-38 的 LS/NSR 或 LS/USR 细胞的 IC 值。通过 RT-PCR 和 HPLC-荧光法分别评估 SN-38 的 mRNA 表达和细胞内 SN-38 积累。LS/USR 细胞中的 IC 值高于 LS/NSR 细胞。LS/USR 细胞中的有机阴离子转运多肽(OATP)2B1 mRNA 表达低于 LS/NSR 细胞,LS/USR 细胞中的 SN-38 积累低于 LS/NSR 细胞。仅共同处理黄芩苷,一种 OATP2B1 抑制剂,几乎消除了 LS/NSR 和 LS/USR 之间 SN-38 积累的差异。OATP2B1 的底物,如 SN-38 的抗癌作用,在相同的血浆底物浓度下,在 ESKD 患者中降低。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3d99/6820778/e354944c5ded/41598_2019_51640_Fig5_HTML.jpg
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