Identification of Aberrant Expression of Gemcitabine-Targeting Proteins in Drug-Resistant Cells Using an Activity-Based Gemcitabine Probe.

IF 3.5 2区 生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Xiaomei Zhu, YuQing Yuan, Kai Wang, Wei Shen, Qing Zhu
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引用次数: 0

Abstract

Gemcitabine-based monotherapy or combination therapy has become the standard treatment for locally advanced and metastatic pancreatic cancer. However, the emergence of resistance within weeks of treatment severely compromises therapeutic efficacy. The intricate biological process of gemcitabine resistance in pancreatic cancer presents a complex challenge, as the underlying mechanisms remain unclear. Identifying the target protein of gemcitabine is crucial for studying its drug-resistance mechanism. An activity-based probe is a powerful tool for studying drug target proteins, but the current lack of activity-based gemcitabine probes with robust biological activity hinders research on gemcitabine. In this study, we developed three active probes based on gemcitabine, among which Gem-3 demonstrated excellent stability and labeling efficacy. We utilized Gem-3 in conjunction with chemical proteomics to identify intracellular target proteins. We identified 79 proteins that interact with gemcitabine, most of which were previously unknown and represented various functional classes. Additionally, we validated the increased expression of IFIT3 and MARCKS in drug-resistant cells, along with the activation of the NF-κB signaling pathway. These findings substantially contribute to our comprehension of gemcitabine's target proteins and further our understanding of the mechanisms driving gemcitabine resistance in pancreatic cancer cells.

利用基于活性的吉西他滨探针识别耐药细胞中吉西他滨靶向蛋白的异常表达
吉西他滨单药或联合疗法已成为治疗局部晚期和转移性胰腺癌的标准疗法。然而,治疗后数周内出现的耐药性严重影响了疗效。吉西他滨在胰腺癌中产生耐药性的生物过程错综复杂,其潜在机制尚不清楚,因此是一项复杂的挑战。确定吉西他滨的靶蛋白对研究其耐药机制至关重要。基于活性的探针是研究药物靶蛋白的有力工具,但目前缺乏具有强大生物活性的基于活性的吉西他滨探针,这阻碍了对吉西他滨的研究。在这项研究中,我们开发了三种基于吉西他滨的活性探针,其中 Gem-3 具有出色的稳定性和标记效果。我们将 Gem-3 与化学蛋白质组学相结合,鉴定了细胞内的靶蛋白。我们发现了 79 种与吉西他滨相互作用的蛋白质,其中大部分是以前未知的,代表了不同的功能类别。此外,我们还验证了耐药细胞中 IFIT3 和 MARCKS 表达的增加,以及 NF-κB 信号通路的激活。这些发现极大地促进了我们对吉西他滨靶蛋白的理解,并进一步加深了我们对胰腺癌细胞吉西他滨耐药机制的认识。
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
ACS Chemical Biology
ACS Chemical Biology 生物-生化与分子生物学
CiteScore
7.50
自引率
5.00%
发文量
353
审稿时长
3.3 months
期刊介绍: ACS Chemical Biology provides an international forum for the rapid communication of research that broadly embraces the interface between chemistry and biology. The journal also serves as a forum to facilitate the communication between biologists and chemists that will translate into new research opportunities and discoveries. Results will be published in which molecular reasoning has been used to probe questions through in vitro investigations, cell biological methods, or organismic studies. We welcome mechanistic studies on proteins, nucleic acids, sugars, lipids, and nonbiological polymers. The journal serves a large scientific community, exploring cellular function from both chemical and biological perspectives. It is understood that submitted work is based upon original results and has not been published previously.
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