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一种构象特异性 ON 开关,可使用口服药物控制 CAR T 细胞。

A conformation-specific ON-switch for controlling CAR T cells with an orally available drug.

机构信息

St. Anna Children's Cancer Research Institute (CCRI), 1090 Vienna, Austria.

Christian Doppler Laboratory for Next Generation CAR T Cells, 1090 Vienna, Austria.

出版信息

Proc Natl Acad Sci U S A. 2020 Jun 30;117(26):14926-14935. doi: 10.1073/pnas.1911154117. Epub 2020 Jun 17.

Abstract

Molecular ON-switches in which a chemical compound induces protein-protein interactions can allow cellular function to be controlled with small molecules. ON-switches based on clinically applicable compounds and human proteins would greatly facilitate their therapeutic use. Here, we developed an ON-switch system in which the human retinol binding protein 4 (hRBP4) of the lipocalin family interacts with engineered hRBP4 binders in a small molecule-dependent manner. Two different protein scaffolds were engineered to bind to hRBP4 when loaded with the orally available small molecule A1120. The crystal structure of an assembled ON-switch shows that the engineered binder specifically recognizes the conformational changes induced by A1120 in two loop regions of hRBP4. We demonstrate that this conformation-specific ON-switch is highly dependent on the presence of A1120, as demonstrated by an ∼500-fold increase in affinity upon addition of the small molecule drug. Furthermore, the ON-switch successfully regulated the activity of primary human CAR T cells in vitro. We anticipate that lipocalin-based ON-switches have the potential to be broadly applied for the safe pharmacological control of cellular therapeutics.

摘要

分子开关是一种能够通过化学化合物诱导蛋白质-蛋白质相互作用的元件,可以实现用小分子来控制细胞功能。基于临床上可应用的化合物和人体蛋白质的分子开关将极大地促进其治疗用途的发展。在这里,我们开发了一种基于亲脂素家族的人视黄醇结合蛋白 4(hRBP4)的分子开关系统,该系统中的 hRBP4 能够与工程化的 hRBP4 结合物在小分子依赖的方式下相互作用。我们设计了两种不同的蛋白质支架,当装载上可口服的小分子 A1120 时,这两种支架能够与 hRBP4 结合。组装好的分子开关的晶体结构表明,工程化的结合物能够特异性地识别 A1120 诱导的 hRBP4 中两个环区的构象变化。我们证明了这种构象特异性的分子开关高度依赖于小分子药物的存在,当加入小分子药物时,亲和力会增加约 500 倍。此外,该分子开关还成功地调节了体外原代人 CAR T 细胞的活性。我们预计基于亲脂素的分子开关具有广泛应用于安全药理学控制细胞治疗的潜力。

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