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首页> 外文期刊>Developmental Immunology: Journal of Immunology Research >Mechanisms and Mediators of Inflammation: Potential Models for Skin Rejection and Targeted Therapy in Vascularized Composite Allotransplantation
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Mechanisms and Mediators of Inflammation: Potential Models for Skin Rejection and Targeted Therapy in Vascularized Composite Allotransplantation

机译:炎症的机制和介导剂:血管化复合同种异体移植中皮肤排斥和靶向治疗的潜在模型

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Vascularized composite allotransplantation (VCA) is an effective treatment option for patients suffering from limb loss or severe disfigurement. However, postoperative courses of VCA recipients have been complicated by skin rejection, and long-term immunosuppression remains a necessity for allograft survival. To widen the scope of this quality-of-life improving procedure minimization of immunosuppression in order to limit risks and side effects is needed. In some aspects, the molecular mechanisms and dynamics of skin allograft rejection seem similar to inflammatory skin conditions. T cells are key players in skin rejection and are recruited to the skin via activation of adhesion molecules, cytokines, and chemokines. Blocking these molecules has not only shown success in the treatment of inflammatory dermatoses, but also prolonged graft survival in various models of solid organ transplantation. In addition to T cell recruitment, ectopic lymphoid structures within the allograft associated with chronic rejection in solid organ transplantation might contribute to the strong alloimmune response towards the skin. Selectively targeting the molecules involved offers exciting novel therapeutic options in the prevention and treatment of skin rejection after VCA.
机译:血管化复合同种异体移植(VCA)对于肢体丢失或严重毁容的患者是一种有效的治疗选择。但是,VCA接受者的术后病程因皮肤排斥而变得复杂,长期免疫抑制仍然是同种异体移植存活的必要条件。为了扩大这种生活质量改善程序的范围,需要最小化免疫抑制以限制风险和副作用。在某些方面,同种异体皮肤排斥反应的分子机制和动力学似乎类似于炎症性皮肤病。 T细胞是皮肤排斥的关键因素,并通过粘附分子,细胞因子和趋化因子的激活而募集到皮肤上。阻断这些分子不仅在炎症性皮肤病的治疗中显示出成功,而且在各种实体器官移植模型中也延长了移植物的存活。除了募集T细胞外,同种异体移植物中的异位淋巴结构与实体器官移植中的慢性排斥反应有关,可能有助于对皮肤的强烈同种异体免疫反应。选择性靶向所涉及的分子为预防和治疗VCA后皮肤排斥反应提供了令人兴奋的新颖治疗选择。

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