Publication | Closed Access
Immune escape of melanoma: first evidence of structural alterations in two distinct components of the MHC class I antigen processing pathway.
189
Citations
16
References
2001
Year
HistocompatibilityMhc ClassImmunologyPathologyAntigen ProcessingInnate ImmunityImmune SystemImmunotherapyTumor ImmunityImmune EscapeImmune SelectionMelanomaCell BiologyTumor MicroenvironmentStructural AlterationsCancer ImmunosurveillanceSignal TransductionBp DeletionHla TypingMedicine
Sequence analyses of the transporter associated with antigen processing (TAP) in tumor cell lines with deficient MHC class I surface expression identified a bp deletion at position 1489 near the ATP-binding domain of Tap1, causing a frameshift in one melanoma cell line. The impaired TAP1 protein expression was associated with deficient TAP2 protein expression, peptide binding, translocation, and MHC class I surface expression. Stable TAP1 gene transfer reconstitutes the described defects, whereas lysis by HLA-A2-restricted CTLs was still abrogated. This was attributable to a 2-bp insertion at position 890 in the HLA-A2 gene and was corrected after HLA-A2 cotransfection. This study describes for the first time mutations in two distinct components of the MHC class I antigen processing pathway, suggesting an immune selection against CTLs recognizing both TAP-dependent and -independent T-cell epitopes.
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