Binding specificity of HuScFv to cholangiocarcinoma cells; New avenues for diagnosis and treatment.

IF 2.3 4区医学 Q3 ALLERGY Asian Pacific journal of allergy and immunology Pub Date : 2024-11-17 DOI:10.12932/AP-210624-1877

Nathawadee Sawatpiboon, Monrat Chulanetra, Wanpen Chaicumpa, Sunisa Duang Sa-Ard, Kanda Kasetsinsombat, Adisak Wongkajornsilp

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Abstract

Background: Cholangiocarcinoma (CCA) is a very aggressive cancer of the bile ducts. Recent advances in immunotherapy, particularly with human single-chain variable fragments (HuScFv), have shown promise in the treatment of solid tumors by targeting cancer cells or improving the immune response.

Objective: This study aimed to select and produce human single-chain antibody fragments (HuScFv) specific to CCA cells (HubCCA1, RMCCA) from phage display HuScFv libraries with minimum or no binding to cholangiocytes (MMNK1).

Methods: Phages that displayed HuScFv to CCA cells were selected by bio-panning and each phagemid was transduced to HB2151 E. coli. The presence of huscfv was determined by direct colony PCR. HuScFv was produced in the E. coli and detected by Western blot analysis and confirmed their specificity and binding capacity to CCA by flow cytometry.

Results: From biopanning, 196 of 350 colonies (56%) of HB2151 E. coli harboring the huscfv gene, and 106 of these (30%) produced the protein. Flow cytometry testing with 14 clones confirmed the presence of the HuScFv protein. The result showed that five HuScFv clones (25, 33, 61, 68, and 80) exhibited stronger binding to CCA cell lines (HubCCA1, RMCCA) compared to cholangiocytes. Furthermore, each clone possessed a distinct amino acid sequence, suggesting unique binding specificities.

Conclusions: HuScFv specific to CCA cells were successfully selected from phage display HuScFv libraries which offer new revenues to develop a pan-CCA immunotherapy and diagnosis of CCA.

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HuScFv 与胆管癌细胞的结合特异性；诊断和治疗的新途径。

背景：胆管癌（CCA）是一种侵袭性极强的胆管癌。免疫疗法的最新进展，特别是人类单链可变片段（HuScFv），通过靶向癌细胞或改善免疫反应，在实体瘤的治疗中显示出前景：本研究旨在从噬菌体展示的HuScFv文库中筛选并制备特异于CCA细胞（HubCCA1、RMCCA）的人类单链抗体片段（HuScFv），同时尽量减少或不与胆管细胞（MMNK1）结合：方法：通过生物淘洗筛选出对 CCA 细胞显示 HuScFv 的噬菌体，并将每种噬菌体转导至 HB2151 大肠杆菌。通过直接菌落 PCR 测定噬菌体是否含有 HuScFv。在大肠杆菌中产生 HuScFv，通过 Western 印迹分析进行检测，并通过流式细胞术确认其特异性和与 CCA 的结合能力：结果：通过生物扫描，HB2151 大肠杆菌的 350 个菌落中有 196 个（56%）携带 huscfv 基因，其中 106 个（30%）产生了该蛋白。对 14 个克隆进行的流式细胞术检测证实了 HuScFv 蛋白的存在。结果显示，与胆管细胞相比，五个 HuScFv 克隆（25、33、61、68 和 80）与 CCA 细胞系（HubCCA1、RMCCA）的结合力更强。此外，每个克隆都具有不同的氨基酸序列，表明它们具有独特的结合特异性：结论：从噬菌体展示HuScFv文库中成功筛选出了特异于CCA细胞的HuScFv，为开发泛CCA免疫疗法和诊断CCA提供了新的途径。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Asian Pacific journal of allergy and immunology 医学-过敏

CiteScore

12.80

自引率

0.00%

发文量

审稿时长

>12 weeks

期刊介绍： The Asian Pacific Journal of Allergy and Immunology (APJAI) is an online open access journal with the recent impact factor (2018) 1.747 APJAI published 4 times per annum (March, June, September, December). Four issues constitute one volume. APJAI publishes original research articles of basic science, clinical science and reviews on various aspects of allergy and immunology. This journal is an official journal of and published by the Allergy, Asthma and Immunology Association, Thailand. The scopes include mechanism, pathogenesis, host-pathogen interaction, host-environment interaction, allergic diseases, immune-mediated diseases, epidemiology, diagnosis, treatment and prevention, immunotherapy, and vaccine. All papers are published in English and are refereed to international standards.