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Emerging cellular and molecular targets in fibrosis: implications for scleroderma pathogenesis and targeted therapy.

机译:纤维化中新兴的细胞和分子靶标:对硬皮病发病机理和靶向治疗的意义。

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摘要

Progress in understanding the cellular, molecular, and biomechanical regulators of fibrosis has led to the identification of novel targets for interrupting the fibrotic process in SSc. Efforts to antagonize cytokine pathways, affect mesenchymal cell fates, attenuate senescence, and clear activated myofibroblasts, along with modifying the ECM mechanical environment, may ultimately lead to effective therapies in SSc.
机译:在了解纤维化的细胞,分子和生物力学调节剂方面的进展已导致鉴定用于中断SSc纤维化过程的新靶标。拮抗细胞因子途径,影响间充质细胞命运,减弱衰老和清除活化的成纤维细胞的努力,以及改变ECM机械环境,最终可能导致SSc的有效治疗。

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