Regulation of HLA Antigen Expression in Human Kidney

PHILIP F. HALLORAN, PETER AUTENRIED, ARTURO WADGYMAR
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引用次数: 5

Abstract

The expression of class II, and even of class I, MHC products in many sites in normal kidney may be low enough to be rate-limiting for antibody-mediated or T cell-mediated injury involving these structures (e.g. rejection). In certain human diseases and in experimental animal models, renal expression of class I and II MHC antigens is capable of large quantitative changes accompanied by shifts in sites of expression. These alterations may be induced by local or systemic processes, and can at times be controlled or reversed by pharmacological intervention (e.g. cyclosporin). The interferons, especially γ-interferon, are probably involved in these changes, but many other influences may also participate. The study of MHC induction may prove to be useful in the clinical and pathological assessment of renal disease, and in understanding the pathogenesis of some forms of renal injury, such as rejection and interstitial nephritis. At present, further studies are needed to unravel the significance of these changes.

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HLA抗原在人肾脏中的表达调控
在正常肾脏的许多部位,II类甚至I类MHC产物的表达可能低到足以限制抗体介导或T细胞介导的涉及这些结构的损伤(例如排斥反应)。在某些人类疾病和实验动物模型中,I类和II类MHC抗原的肾脏表达能够发生大量的定量变化,并伴有表达位点的转移。这些改变可由局部或全身过程引起,有时可通过药物干预(如环孢素)加以控制或逆转。干扰素,尤其是γ-干扰素,可能参与了这些变化,但许多其他影响也可能参与其中。MHC诱导的研究可能有助于肾脏疾病的临床和病理评估,并有助于了解某些肾损伤的发病机制,如排斥反应和间质性肾炎。目前,需要进一步的研究来揭示这些变化的意义。
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