首页> 外文期刊>American Journal of Pathology: Official Publication of the American Association of Pathologists >An experimental model of acute humoral rejection of renal allografts associated with concomitant cellular rejection.
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An experimental model of acute humoral rejection of renal allografts associated with concomitant cellular rejection.

机译:与伴随细胞排斥相关的肾同种异体移植物急性体液排斥的实验模型。

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摘要

Acute humoral rejection (AHR), which occurs in up to 8 of kidney transplant recipients, is a significant cause of renal allograft dysfunction and loss. More efficacious treatment modalities are needed to eliminate or curtail alloantibody production and its deleterious effects on the kidney. The availability of animal models mimicking human AHR is essential to understand its pathophysiology and develop new treatment strategies. Using a mouse kidney transplant model, we demonstrate that presensitization of recipients with donor skin grafts results in rejection of subsequent renal allografts. All presensitized mice developed renal failure 8.6 +/- 4.3 days after engraftment, with serum creatinine values near 100 micromol/dl. Graft histology revealed mild, diffuse, interstitial, mononuclear cell infiltrates; prominent peritubular capillary inflammatory cell margination; patchy interstitial hemorrhage; interstitial edema; and focal glomerular fibrin deposition. Complement (C3d) deposition was diffuse and prominent in peritubular capillaries. Serum analysis demonstrated high levels of circulating alloantibodies with broad cross-reactivity to many MHC haplotypes. The clinical setting and histological findings of our model strongly resemble AHR, which is frequently associated with cellular rejection, a situation commonly encountered in human renal allograft recipients. This animal model provides a valuable tool to study the pathogenesis of AHR, its relationship to cellular alloimmunity, its contribution to graft injury, and the effects of various potential therapeutic interventions.
机译:急性体液排斥反应 (AHR) 发生于高达 8% 的肾移植受者中,是同种异体肾移植物功能障碍和丢失的重要原因。需要更有效的治疗方式来消除或减少同种抗体的产生及其对肾脏的有害影响。模拟人类AHR的动物模型的可用性对于了解其病理生理学和开发新的治疗策略至关重要。使用小鼠肾移植模型,我们证明接受者与供体皮肤移植物的早敏导致随后的肾同种异体移植物排斥。所有早致敏小鼠在植入后 8.6 +/- 4.3 天出现肾功能衰竭,血清肌酐值接近 100 μmol/dl。移植物组织学显示轻度、弥漫性间质性单核细胞浸润;突出的肾小管周围毛细血管炎性细胞边缘;斑片状间质出血;间质性水肿;和局灶性肾小球纤维蛋白沉积。补体 (C3d) 沉积在肾小管周围毛细血管中弥漫且突出。血清分析显示,循环同种异体抗体水平高,对许多 MHC 单倍型具有广泛的交叉反应性。我们模型的临床环境和组织学结果与AHR非常相似,AHR通常与细胞排斥有关,这是人类同种异体肾移植受者中常见的情况。该动物模型为研究AHR的发病机制、其与细胞同种免疫的关系、其对移植物损伤的贡献以及各种潜在治疗干预措施的效果提供了有价值的工具。

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