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The Potential of MicroRNAs as Novel Biomarkers for Transplant Rejection

机译:MicroRNAs作为新型生物标志物的移植排斥的潜力。

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摘要

The control of gene expression by microRNAs (miRNAs, miR) influences many cellular functions, including cellular differentiation, cell proliferation, cell development, and functional regulation of the immune system. Recently, miRNAs have been detected in serum, plasma, and urine and circulating miR profiles have been associated with a variety of diseases. Rejection is one of the major causes of allograft failure and preventing and treating acute rejection are the central task for clinicians working with transplant patients. Invasive biopsies used in monitoring rejection are burdensome and risky to transplant patients. Novel and easily accessible biomarkers of acute rejection could make it possible to detect rejection earlier and make more fine-tuned calibration of immunosuppressive or new target treatment possible. In this review, we discuss whether circulating miRNA can serve as an early noninvasive diagnostic biomarker and an expression fingerprint of allograft rejection and transplant failure. Understanding the regulatory interplay of relevant miRNAs and the rejecting allograft will result in a better understanding of the molecular pathophysiology of alloimmune injury.
机译:microRNA(miRNA,miR)对基因表达的控制影响许多细胞功能,包括细胞分化,细胞增殖,细胞发育以及免疫系统的功能调节。最近,已在血清,血浆和尿液中检测到miRNA,并且循环miR谱已与多种疾病相关。排斥是同种异体移植失败的主要原因之一,预防和治疗急性排斥反应是与移植患者一起工作的临床医生的主要任务。用于监测排斥反应的有创活检对移植患者而言是繁重且有风险的。新型且易于获得的急性排斥反应生物标志物,可以更早地检测排斥反应,并可以对免疫抑制或新的靶标治疗进行更精细的校准。在这篇综述中,我们讨论了循环的miRNA是否可以作为早期的非侵入性诊断生物标志物以及同种异体移植排斥和移植失败的表达指纹。了解相关miRNA和排斥同种异体移植物之间的调控相互作用,将使人们更好地了解同种免疫损伤的分子病理生理学。

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