Antígenos MICA y trasplante / MICA antigens and transplantation

Los antígenos leucocitarios humanos (HLA, del inglés human leukocyte antigens), codificados por los genes del complejo principal de histocompatibilidad (MHC, del inglés m ajor histocompatibility complex), actúan como inductores de las respuestas inmunitarias en el trasplante; sin embargo, los productos de los genes relacionados a cadenas MHC clase I (MIC, del inglés MHC class I chain-related genes), constituyen también uno de los blancos del rechazo. La familia de los genes MIC consta de siete miembros, de los cuales solo MICA y MICB son funcionales. Los transcriptos son glicoproteínas de superficie celular de 62 kDA que presentan homología en su secuencia con las moléculas HLA clase I y cuya función está relacionada con la inmunidad innata. En los órganos trasplantados ocurre un incremento en la expresión de los antígenos MICA como una señal temprana de "peligro" debido al trauma quirúrgico y la isquemia. Esta sobrexpresión antigénica puede llevar al rechazo mediado por anticuerpos anti-MICA que activan el complemento y por un incremento de la citotoxicidad debido a la estimulación en los linfocitos citolíticos naturales (NK, del inglés natural killer) y los linfocitos CD8+ &+ αß y γδ, del receptor conocido como NKG2D (NK grupo 2 miembro D(AU)

Human leukocyte antigens (HLA), encoded by major histocompatibility complex (MHC) genes, act as inducers of immune responses in transplantation. However, the products of the genes related to MHC class I chains (MIC) are also one of the targets of rejection. The family of MIC genes consists of seven members, of which only MICA and MICB are functional. Transcripts are cell surface glycoproteins of 62 kDa that exhibit homology in sequence with HLA class I molecules and whose function is related to innate immunity. In transplanted organs an increase in the expression of MICA antigens occurs as an early sign of "danger" due to surgical trauma and ischemia. This antigenic overexpression can lead to rejection mediated by complement-activating anti-MICA antibodies and by increased cytotoxicity due to stimulation in natural killer (NK) lymphocytes and CD8 + + αß and γδ lymphocytes. Receptor known as NKG2D (NK group 2 member D)(AU)

Ethanol-dependent expression of the NKG2D ligands MICA/B in human cell lines and leukocytes.

Alcohol consumption affects the human immune system, causing a variety of disorders. However, the mechanisms of development of these changes are not fully understood. We hypothesized that ethanol may influence the expression of MICA and MICB, stress-induced molecules capable of regulating the activity of cytotoxic lymphocytes through the interaction with receptor NKG2D, which substantially affects the functionality of cellular immunity. We analyzed the effects of ethanol on MICA/B expression in tumor cell lines and human leukocytes. In the cell line models, ethanol caused different changes in the surface expression of MICA/B; in particular, it induced the translocation of intracellular proteins MICA/B to the cell surface and shedding of MICA (in soluble and microparticle-associated forms) from the plasma membrane. The observed results are not linked with cell death in cultures, taking place only under higher doses of ethanol. Ethanol at physiologically relevant concentrations (and higher) stimulated expression of MICA/B genes in different cell types. The effect of ethanol was more pronounced in hepatocyte line HepG2 compared with hematopoietic cell lines K562, Jurkat, and THP-1. Among the tested leukocytes, the most sensitive to ethanol action were T cells activated ex vivo with IL-2, in which the increase of MICA/B mRNA expression was registered with the smallest dose of ethanol (0.125%). In human monocytes, ethanol may lead to elevations in surface MICA/B levels. Presumably, changes in MICA/B expression caused by ethanol can affect the functions of NKG2D-positive cytotoxic lymphocytes, modulating immune reactions at excessive alcohol consumption.