Make the right measurement: Discovery of an allosteric inhibition site for p300-HAT

IF 2.3 2区物理与天体物理 Q3 CHEMISTRY, PHYSICAL Structural Dynamics-Us Pub Date : 2019-09-01 DOI:10.1063/1.5119336

A. Gardberg, Annissa J Huhn, R. Cummings, A. Bommi-Reddy, F. Poy, J. Setser, V. Vivat, F. Brucelle, Jonathan E. Wilson

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引用次数: 5

Abstract

Histone acetyltransferases (HATs) and histone deacetylases (HDACs) catalyze the dynamic and reversible acetylation of proteins, an epigenetic regulatory mechanism associated with multiple cancers. Indeed, HDAC inhibitors are already approved in the clinic. The HAT paralogs p300 and CREB-binding protein (CBP) have been implicated in human pathological conditions including several hematological malignancies and androgen receptor-positive prostate cancer. Others have reported CoA-competitive inhibitors of p300 and CBP with cell-based activity. Here, we describe 2 compounds, CPI-076 and CPI-090, discovered through p300-HAT high throughput screening screening, which inhibit p300-HAT via binding at an allosteric site. We present the high resolution (1.7 and 2.3 Å) co-crystal structures of these molecules bound to a previously undescribed allosteric site of p300-HAT. Derivatization yielded actionable structure-activity relationships, but the full-length enzymatic assay demonstrated that this allosteric HAT inhibitor series was artifactual, inhibiting only the HAT domain of p300 with no effect on the full-length enzyme.

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进行正确的测量：发现p300 HAT的变构抑制位点

组蛋白乙酰转移酶（HATs）和组蛋白脱乙酰酶（HDAC）催化蛋白质的动态和可逆乙酰化，这是一种与多种癌症相关的表观遗传学调控机制。事实上，HDAC抑制剂已经在临床上获得批准。HAT旁系基因p300和CREB-结合蛋白（CBP）与人类病理状况有关，包括几种血液系统恶性肿瘤和雄激素受体阳性前列腺癌症。其他人报道了具有细胞活性的p300和CBP的CoA竞争性抑制剂。在这里，我们描述了通过p300HAT高通量筛选发现的两种化合物，CPI-076和CPI-090，它们通过变构位点的结合抑制p300HAt。我们展示了高分辨率（1.7和2.3 Å）共晶结构结合到先前未描述的p300HAT变构位点。衍生产生了可操作的构效关系，但全长酶测定表明，该变构HAT抑制剂系列是人为的，仅抑制p300的HAT结构域，对全长酶没有影响。

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

Structural Dynamics-Us CHEMISTRY, PHYSICALPHYSICS, ATOMIC, MOLECU-PHYSICS, ATOMIC, MOLECULAR & CHEMICAL

CiteScore

5.50

自引率

3.60%

发文量

审稿时长

16 weeks

期刊介绍： Structural Dynamics focuses on the recent developments in experimental and theoretical methods and techniques that allow a visualization of the electronic and geometric structural changes in real time of chemical, biological, and condensed-matter systems. The community of scientists and engineers working on structural dynamics in such diverse systems often use similar instrumentation and methods. The journal welcomes articles dealing with fundamental problems of electronic and structural dynamics that are tackled by new methods, such as: Time-resolved X-ray and electron diffraction and scattering, Coherent diffractive imaging, Time-resolved X-ray spectroscopies (absorption, emission, resonant inelastic scattering, etc.), Time-resolved electron energy loss spectroscopy (EELS) and electron microscopy, Time-resolved photoelectron spectroscopies (UPS, XPS, ARPES, etc.), Multidimensional spectroscopies in the infrared, the visible and the ultraviolet, Nonlinear spectroscopies in the VUV, the soft and the hard X-ray domains, Theory and computational methods and algorithms for the analysis and description of structuraldynamics and their associated experimental signals. These new methods are enabled by new instrumentation, such as: X-ray free electron lasers, which provide flux, coherence, and time resolution, New sources of ultrashort electron pulses, New sources of ultrashort vacuum ultraviolet (VUV) to hard X-ray pulses, such as high-harmonic generation (HHG) sources or plasma-based sources, New sources of ultrashort infrared and terahertz (THz) radiation, New detectors for X-rays and electrons, New sample handling and delivery schemes, New computational capabilities.