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小分子通过选择性抑制 BMP1 依赖性 Chordin 切割对 BMP 信号的抑制作用。

Small-Molecule-Mediated Suppression of BMP Signaling by Selective Inhibition of BMP1-Dependent Chordin Cleavage.

机构信息

Graduate School of Pharmaceutical Science, Chiba University, 1-8-1 Inohana, Chuo-ku, Chiba 260-8675, Japan.

Graduate School of Pharmaceutical Sciences, Nagoya University, Furocho, Chikusa, Nagoya 464-8601, Aichi, Japan.

出版信息

Int J Mol Sci. 2023 Feb 21;24(5):4313. doi: 10.3390/ijms24054313.

Abstract

BMP signaling is critical for many biological processes. Therefore, small molecules that modulate BMP signaling are useful for elucidating the function of BMP signaling and treating BMP signaling-related diseases. Here, we performed a phenotypic screening in zebrafish to examine the in vivo effects of N-substituted-2-amino-benzoic acid analogs NPL1010 and NPL3008 and found that they affect BMP signaling-dependent dorsal-ventral (D-V) patterning and bone formation in zebrafish embryos. Furthermore, NPL1010 and NPL3008 suppressed BMP signaling upstream of BMP receptors. BMP1 cleaves Chordin, an antagonist of BMP, and negatively regulates BMP signaling. Docking simulations demonstrated that NPL1010 and NPL3008 bind BMP1. We found that NPL1010 and NPL3008 partially rescued the disruptions in the D-V phenotype caused by overexpression and selectively inhibited BMP1-dependent Chordin cleavage. Therefore, NPL1010 and NPL3008 are potentially valuable inhibitors of BMP signaling that act through selective inhibition of Chordin cleavage.

摘要

BMP 信号对于许多生物过程至关重要。因此,调节 BMP 信号的小分子对于阐明 BMP 信号的功能和治疗 BMP 信号相关疾病非常有用。在这里,我们在斑马鱼中进行了表型筛选,以研究 N-取代-2-氨基苯甲酸类似物 NPL1010 和 NPL3008 的体内作用,发现它们影响斑马鱼胚胎中 BMP 信号依赖性背腹 (D-V) 模式形成和骨骼形成。此外,NPL1010 和 NPL3008 抑制了 BMP 受体上游的 BMP 信号。BMP1 切割 Chordin,一种 BMP 的拮抗剂,负调控 BMP 信号。对接模拟表明,NPL1010 和 NPL3008 与 BMP1 结合。我们发现,NPL1010 和 NPL3008 部分挽救了 过表达引起的 D-V 表型紊乱,并选择性抑制了 BMP1 依赖性 Chordin 切割。因此,NPL1010 和 NPL3008 可能是 BMP 信号的有价值抑制剂,通过选择性抑制 Chordin 切割起作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/555d/10001940/61908f9b043f/ijms-24-04313-g001.jpg

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