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鉴定与雌激素受体α相关的 ChIP-seq 和 RIME 级抗体。

Identification of ChIP-seq and RIME grade antibodies for Estrogen Receptor alpha.

机构信息

Cancer Research UK Cambridge Institute, University of Cambridge, Robinson Way, Cambridge, United Kingdom.

出版信息

PLoS One. 2019 Apr 10;14(4):e0215340. doi: 10.1371/journal.pone.0215340. eCollection 2019.

Abstract

Estrogen Receptor alpha (ERα) plays a major role in most breast cancers, and it is the target of endocrine therapies used in the clinic as standard of care for women with breast cancer expressing this receptor. The two methods ChIP-seq (chromatin immunoprecipitation coupled with deep sequencing) and RIME (Rapid Immunoprecipitation of Endogenous Proteins) have greatly improved our understanding of ERα function during breast cancer progression and in response to anti-estrogens. A critical component of both ChIP-seq and RIME protocols is the antibody that is used against the bait protein. To date, most of the ChIP-seq and RIME experiments for the study of ERα have been performed using the sc-543 antibody from Santa Cruz Biotechnology. However, this antibody has been discontinued, thereby severely impacting the study of ERα in normal physiology as well as diseases such as breast cancer and ovarian cancer. Here, we compare the sc-543 antibody with other commercially available antibodies, and we show that 06-935 (EMD Millipore) and ab3575 (Abcam) antibodies can successfully replace the sc-543 antibody for ChIP-seq and RIME experiments.

摘要

雌激素受体 alpha(ERα)在大多数乳腺癌中起着重要作用,它是临床内分泌治疗的靶点,也是表达这种受体的乳腺癌女性的标准治疗方法。ChIP-seq(染色质免疫沉淀结合深度测序)和 RIME(内源性蛋白快速免疫沉淀)这两种方法极大地提高了我们对 ERα 在乳腺癌进展过程中以及对抗雌激素反应时的功能的理解。ChIP-seq 和 RIME 方案的一个关键组成部分是针对诱饵蛋白的抗体。迄今为止,大多数用于研究 ERα 的 ChIP-seq 和 RIME 实验都是使用来自 Santa Cruz Biotechnology 的 sc-543 抗体进行的。然而,这种抗体已经停产,这严重影响了 ERα 在正常生理以及乳腺癌和卵巢癌等疾病中的研究。在这里,我们比较了 sc-543 抗体与其他市售抗体,并表明 06-935(EMD Millipore)和 ab3575(Abcam)抗体可以成功替代 sc-543 抗体用于 ChIP-seq 和 RIME 实验。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/601c/6457525/b28cd0933c2c/pone.0215340.g001.jpg

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