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Rho GTPase/Rho kinase inhibition as a novel target for the treatment of glaucoma.

机译:Rho GTPase / Rho激酶抑制作为治疗青光眼的新靶标。

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摘要

Rho kinase (ROCK1 and ROCK2) is a serine/threonine kinase that serves as an important downstream effector of Rho GTPase, and plays a critical role in regulating the contractile tone of smooth muscle tissues in a calcium-independent manner. Several lines of experimental evidence indicate that modulating ROCK activity within the aqueous humor outflow pathway using selective inhibitors could achieve very significant benefits for the treatment of increased intraocular pressure in patients with glaucoma. The rationale for such an approach stems from experimental data suggesting that both ROCK and Rho GTPase inhibitors can increase aqueous humor drainage through the trabecular meshwork, leading to a decrease in intraocular pressure. In addition to their ocular hypotensive properties, inhibitors of both ROCK and Rho GTPase have been shown to enhance ocular blood flow, retinal ganglion cell survival and axon regeneration. These properties of the ROCK and Rho GTPase inhibitors indicate that targeting the Rho GTPase/ROCK pathway with selective inhibitors represents a novel therapeutic approach aimed at lowering increased intraocular pressure in glaucoma patients.
机译:Rho激酶(ROCK1和ROCK2)是一种丝氨酸/苏氨酸激酶,是Rho GTPase的重要下游效应子,在以钙非依赖性方式调节平滑肌组织的收缩音中起关键作用。几行实验证据表明,使用选择性抑制剂调节房水流出途径内的ROCK活性对于治疗青光眼患者眼内压增高可能具有非常显着的益处。这种方法的基本原理来自实验数据,表明ROCK和Rho GTPase抑制剂均可增加通过小梁网的房水引流,从而降低眼内压。除具有降眼压作用外,ROCK和Rho GTPase抑制剂均已显示可增强眼血流量,视网膜神经节细胞存活和轴突再生。 ROCK和Rho GTPase抑制剂的这些特性表明,以选择性抑制剂靶向Rho GTPase / ROCK途径代表了一种旨在降低青光眼患者眼内压升高的新型治疗方法。

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