体外免疫预防生肌干细胞激活剂 HGF 的硝化/功能障碍,为老年性肌肉萎缩制定策略

IF 7.8 1区 医学 Q1 Biochemistry, Genetics and Molecular Biology
Aging Cell Pub Date : 2024-09-19 DOI:10.1111/acel.14337
Sakiho Tanaka, Alaa Elgaabari, Miyumi Seki, So Kuwakado, Kahona Zushi, Junri Miyamoto, Shoko Sawano, Wataru Mizunoya, Kenshiro Ehara, Naruha Watanabe, Yohei Ogawa, Hikaru Imakyure, Reina Fujimaru, Rika Osaki, Kazuki Shitamitsu, Kaoru Mizoguchi, Tomoki Ushijima, Takahiro Maeno, Takashi Nakashima, Takahiro Suzuki, Mako Nakamura, Judy E. Anderson, Ryuichi Tatsumi
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引用次数: 0

摘要

针对过氧化亚硝酸盐(ONOO-)的产生,肌源性干卫星细胞激活剂 HGF(肝细胞生长因子)主要在快 IIa 和 IIx 肌纤维上的酪氨酸残基(Y198 和 Y250)发生硝化,从而失去与信号受体 c-met 的结合,从而在衰老过程中扰乱肌肉稳态。在这里,我们发现了大鼠抗 HGF 单克隆抗体(mAb)1H41C10,该抗体是针对在哺乳动物中保存完好的合成肽 FTSNPEVRnitroY198EV(该位点在 HGF 上具有抗硝化功能障碍的功能)而自行培养的。Western 印迹法显示,1H41C10 能识别硝化和非硝化的 HGF,并具有不同的亲和力,这表明 1H41C10 的副肽可能与 Y198 的邻近位点结合。随后的实验表明,与 1H41C10 结合的 HGF 能抵抗过亚硝酸盐诱导的 Y198 硝化。与之配套的 mAb-1H42F4 具有类似的免疫反应性,但不能保护 Y198 硝化,因此可作为对照。重要的是,1H41C10-HGF 还经受住了 Y250 的硝化,在培养过程中保留了 c-met 结合和卫星细胞活化功能。1H41C10 的 Fab 区对 Y250 硝化具有抵抗力,这可能是由于它定位在紧邻 Y250 的位置,另外一组实验也证明了这一点,该实验表明 1H41C10-Fab 对 Y250 硝化具有抵抗力,而 Fc 区段则没有。研究结果突显了 1H41C10 对 HGF 硝化功能障碍的体外预防性影响,这种功能障碍会严重损害成肌干细胞的活力,有可能为抗衡或治疗与纤维化(包括肌肉疏松症和虚弱症)有关的老年性肌肉萎缩以及研究性 HGF 药物的治疗应用开创出令人信服的策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

In vitro immuno-prevention of nitration/dysfunction of myogenic stem cell activator HGF, towards developing a strategy for age-related muscle atrophy

In vitro immuno-prevention of nitration/dysfunction of myogenic stem cell activator HGF, towards developing a strategy for age-related muscle atrophy

In vitro immuno-prevention of nitration/dysfunction of myogenic stem cell activator HGF, towards developing a strategy for age-related muscle atrophy

In response to peroxynitrite (ONOO) generation, myogenic stem satellite cell activator HGF (hepatocyte growth factor) undergoes nitration of tyrosine residues (Y198 and Y250) predominantly on fast IIa and IIx myofibers to lose its binding to the signaling receptor c-met, thereby disturbing muscle homeostasis during aging. Here we show that rat anti-HGF monoclonal antibody (mAb) 1H41C10, which was raised in-house against a synthetic peptide FTSNPEVRnitroY198EV, a site well-conserved in mammals, functions to confer resistance to nitration dysfunction on HGF. 1H41C10 was characterized by recognizing both nitrated and non-nitrated HGF with different affinities as revealed by Western blotting, indicating that the paratope of 1H41C10 may bind to the immediate vicinity of Y198. Subsequent experiments showed that 1H41C10-bound HGF resists peroxynitrite-induced nitration of Y198. A companion mAb-1H42F4 presented similar immuno-reactivity, but did not protect Y198 nitration, and thus served as the control. Importantly, 1H41C10-HGF also withstood Y250 nitration to retain c-met binding and satellite cell activation functions in culture. The Fab region of 1H41C10 exerts resistivity to Y250 nitration possibly due to its localization in the immediate vicinity to Y250, as supported by an additional set of experiments showing that the 1H41C10-Fab confers Y250-nitration resistance which the Fc segment does not. Findings highlight the in vitro preventive impact of 1H41C10 on HGF nitration-dysfunction that strongly impairs myogenic stem cell dynamics, potentially pioneering cogent strategies for counteracting or treating age-related muscle atrophy with fibrosis (including sarcopenia and frailty) and the therapeutic application of investigational HGF drugs.

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来源期刊
Aging Cell
Aging Cell 生物-老年医学
CiteScore
14.40
自引率
2.60%
发文量
212
审稿时长
8 weeks
期刊介绍: Aging Cell, an Open Access journal, delves into fundamental aspects of aging biology. It comprehensively explores geroscience, emphasizing research on the mechanisms underlying the aging process and the connections between aging and age-related diseases.
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