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CMX001 potentiates the efficacy of acyclovir in herpes simplex virus infections.

机译:CMX001增强了阿昔洛韦在单纯疱疹病毒感染中的功效。

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Although acyclovir (ACV) has proven to be of value in the therapy of certain herpes simplex virus (HSV) infections, there is a need for more effective therapies, particularly for serious infections in neonates and immunocompromised individuals, where resistance to this drug can be problematic. CMX001 is an orally bioavailable lipid conjugate of cidofovir that is substantially less nephrotoxic than the parent drug and has excellent antiviral activity against all the human herpesviruses. This compound retains full antiviral activity against ACV-resistant laboratory and clinical isolates. The combined efficacy of CMX001 and ACV was evaluated in a new real-time PCR combination assay, which demonstrated that the combination synergistically inhibited the replication of HSV in cell culture. This was also confirmed in murine models of HSV infection, where the combined therapy with these two drugs synergistically reduced mortality. These results suggest that CMX001 may be effective in the treatment of ACV-resistant HSV infections and as an adjunct therapy in individuals with suboptimal responses to ACV.
机译:尽管已证明阿昔洛韦(ACV)在某些单纯疱疹病毒(HSV)感染的治疗中具有价值,但仍需要更有效的疗法,尤其是对于新生儿和免疫功能低下的个体中的严重感染,在这种情况下,该药可能会产生耐药性有问题的。 CMX001是西多福韦的口服生物利用脂质结合物,其肾毒性远低于母体药物,并且对所有人类疱疹病毒具有出色的抗病毒活性。该化合物对抗ACV的实验室和临床分离株具有完全的抗病毒活性。在新的实时PCR组合测定中评估了CMX001和ACV的联合疗效,证明了该组合协同抑制了HSV在细胞培养物中的复制。在HSV感染的鼠模型中也证实了这一点,其中两种药物的联合治疗可协同降低死亡率。这些结果表明,CMX001可有效治疗耐ACV的HSV感染,并可作为对ACV反应欠佳的个体的辅助治疗。

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