March 3, 2026Open Access

Calreticulin-Mediated Quality Control of the Non-Classical MHC-I Molecule MICA: Implications for Immune Surveillance

Key Points

MICA retention in melanoma cells indicates a crucial role in immune surveillance, with potential implications for treatment.
Immunoprecipitation assays show that calreticulin preferentially associates with low-molecular-weight MICA forms.
Analysis of recombinant proteins reveals how calreticulin interacts with non-glycosylated MICA but not fully glycosylated forms.
Findings suggest that dysregulation of calreticulin-dependent MICA retention may facilitate immune evasion in melanoma.

Abstract

Major histocompatibility complex class I chain-related gene A (MICA) is a non-classical MHC-I molecule essential for immune surveillance, yet its intracellular maturation remains poorly understood. We show that MICA is predominantly retained intracellularly in melanoma cells and colocalizes with the endoplasmic reticulum chaperone calreticulin (CRT). Notably, MICA also colocalizes with CRT in healthy skin. Immunoprecipitation assays reveal that CRT preferentially associates with a low-molecular-weight form of MICA. Recombinant protein assays and in silico analyses support direct interaction between CRT and non-glycosylated MICA, but not with fully glycosylated eukaryotic MICA. These findings identify CRT-dependent retention of MICA as a physiological checkpoint that may be dysregulated in melanoma to promote immune evasion.

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Calreticulin-Mediated Quality Control of the Non-Classical MHC-I Molecule MICA: Implications for Immune Surveillance

Key Points

Abstract

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