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A tropism-modified adenoviral vector increased the effectiveness of gene therapy for arthritis.

机译:向性修饰的腺病毒载体提高了关节炎基因治疗的有效性。

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Adenoviral vectors (AdV) are used for anti-inflammatory cytokine therapy in experimental arthritis. Cell entry of AdV is dependent on the initial recognition of the coxsackie-adenovirus receptor (CAR) on cells. Recently, an Arg-Gly-Asp (RGD) motif was introduced in the HI loop of the fiber knob, this enables the adenovirus to bypass CAR and mediate cell entry via RGD binding integrins. In this study, we explored the transduction efficiency of the RGD-modified adenovirus in synovium and compared the RGD-modified with the conventional adenoviral vector for their effectiveness to modulate the murine collagen-induced arthritis (CIA) model when used to overexpress mIL-1Ra in the knee joint. Twenty-four hours after intra-articular injection of 10(7) fluorescent forming units (ffu) virus, luciferase (luc) activity in Ad5LucRGD-injected joints was up to 38 times higher than in AdCMVLuc-injected joints, and in arthritic joints the transduction efficiency was up to 69 times higher for the Ad5LucRGD viruses. Transduction of the synovial lining by the RGD-modified adenovirus containing the mIL-1Ra transgene, markedly improved the inhibition of CIA compared with the conventional virus in both a prophylactic and therapeutic treatment protocol. These results show that targeting integrins with the RGD-modified AdV improved the outcome of gene therapy for arthritis.
机译:腺病毒载体(AdV)用于实验性关节炎的抗炎细胞因子治疗。 AdV的细胞进入取决于细胞上柯萨奇腺病毒受体(CAR)的初始识别。最近,在纤维瘤的HI环中引入了Arg-Gly-Asp(RGD)基序,这使腺病毒能够绕过CAR并通过RGD结合整联蛋白介导细胞进入。在这项研究中,我们探讨了RGD修饰的腺病毒在滑膜中的转导效率,并比较了RGD修饰的腺病毒与常规腺病毒载体在过表达mIL-1Ra时调节鼠胶原诱导的关节炎(CIA)模型的有效性。在膝盖关节。关节内注射10(7)荧光形成单位(ffu)病毒后二十四小时,注射Ad5LucRGD的关节中的荧光素酶(luc)活性比注射AdCMVLuc的关节和关节炎关节中的荧光素酶高38倍。 Ad5LucRGD病毒的转导效率高达69倍。在预防和治疗方案中,与常规病毒相比,包含mIL-1Ra转基因的RGD修饰的腺病毒对滑膜衬里的转导显着改善了CIA的抑制作用。这些结果表明,用RGD修饰的AdV靶向整联蛋白可改善关节炎基因治疗的效果。

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