AP-1 Mediates Cellular Adaptation and Memory Formation During Therapy Resistance

bioRxiv - Systems Biology Pub Date : 2024-07-25 DOI:10.1101/2024.07.25.604999

Jingxin Li, Pavithran T. Ravindran, Aoife O'Farrell, Gianna T. Busch, Ryan H. Boe, Zijian Niu, Sean Woo, Maraget C. Dunagin, Naveen Jain, Yogesh Goyal, Kavitha Sarma, Meenhard Herlyn, Arjun Raj

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Abstract

Cellular responses to environmental stimuli are typically thought to be governed by genetically encoded programs. We demonstrate that melanoma cells can form and maintain cellular memories during the acquisition of therapy resistance that exhibit characteristics of cellular learning and are dependent on the transcription factor AP-1. We show that cells exposed to a low dose of therapy adapt to become resistant to a high dose, demonstrating that resistance was not purely selective. The application of therapy itself results in the encoding of transient gene expression into cellular memory and that this encoding occurs for both transiently induced and probabilistically arising expression. Chromatin accessibility showed concomitant persistence. A two-color AP-1 reporter system showed that these memories are encoded in cis, constituting an example of activating cis epigenetics. Our findings establish the formation and maintenance of cellular memories as a critical aspect of gene regulation during the development of therapy resistance.

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AP-1 在治疗抵抗过程中介导细胞适应和记忆形成

细胞对环境刺激的反应通常被认为是由基因编码程序控制的。我们的研究表明，黑色素瘤细胞在获得抗药性的过程中可以形成并维持细胞记忆，这种记忆表现出细胞学习的特征，并且依赖于转录因子 AP-1。我们发现，接受低剂量治疗的细胞会适应高剂量治疗，从而产生抗药性，这表明抗药性并非纯粹是选择性的。应用治疗本身会将瞬时基因表达编码为细胞记忆，而且这种编码同时发生在瞬时诱导表达和概率性表达上。染色质的可及性同时显示出持久性。双色 AP-1 报告系统显示，这些记忆是顺式编码的，是激活顺式表观遗传学的一个实例。我们的研究结果表明，细胞记忆的形成和维持是耐药性形成过程中基因调控的一个重要方面。

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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bioRxiv - Systems Biology

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