Selective Histocompatibility Leukocyte Antigen (HLA)-A2 Loss Caused by Aberrant Pre-mRNA Splicing in 624MEL28 Melanoma Cells

doi:10.1084/jem.190.2.205

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J. Exp. Med., Volume 190, Number 2, July 19, 1999 205-216
Copyright © 1999 by The Rockefeller University Press.

Selective Histocompatibility Leukocyte Antigen (HLA)-A2 Loss Caused by Aberrant Pre-mRNA Splicing in 624MEL28 Melanoma Cells

Zhigang Wang^a, Francesco M. Marincola^b, Licia Rivoltini^c, Giorgio Parmiani^c, and Soldano Ferrone^a
^a From the Department of Immunology, Roswell Park Cancer Institute, Buffalo, New York 14263
^b Surgery Branch, Division of Clinical Sciences, National Cancer Institute, and the HLA Laboratory, Department of Transfusion Medicine, Clinical Center, National Institutes of Health, Bethesda, Maryland 20892
^c Division of Experimental Oncology D, Istituto Nazionale dei Tumori, 20133 Milan, Italy

Correspondence to: Soldano Ferrone, Department of Immunology, Roswell Park Cancer Institute, Elm and Carlton Sts., Buffalo, NY 14263., ferrone{at}sc3102.med.buffalo.edu (E-mail), 716-845-8534 (phone), 716-845-8906 (fax)

Histocompatibility leukocyte antigen (HLA)-A2 is used as a restrictingelement to present several melanoma-associated antigen (MAA)-derivedpeptides to cytotoxic T lymphocytes (CTLs). HLA-A2 antigen isselectively lost in primary melanoma lesions and more frequentlyin metastases. Only scanty information is available about themolecular mechanisms underlying this abnormality, in spite ofits potentially negative impact on the clinical course of thedisease and on the outcome of T cell–based immunotherapy.Therefore, in this study we have shown that the selective HLA-A2antigen loss in melanoma cells 624MEL28 is caused by a splicingdefect of HLA-A2 pre-mRNA because of a base substitution atthe 5' splice donor site of intron 2 of the HLA-A2 gene. Asa result, HLA-A2 transcripts are spliced to two aberrant forms,one with exon 2 skipping and the other with intron 2 retention.The latter is not translated because of an early premature stopcodon in the retained intron. In contrast, the transcript withexon 2 skipping is translated to a truncated HLA-A2 heavy chainwithout the ${alpha}$ ₁ domain. Such a polypeptide is synthesized in vitrobut is not detectable in cells, probably because of the lowsteady state level of the corresponding mRNA and the low translationefficiency. These results indicate that a single mutationalevent in an HLA class I gene is sufficient for loss of the correspondingallele. This may account, at least in part, for the high frequencyof selective HLA class I allele loss in melanoma cells. Ourconclusion emphasizes the need to implement active specificimmunotherapy with a combination of peptides presented by variousHLA class I alleles. This strategy may counteract the abilityof melanoma cells with selective HLA class I allele loss toescape from immune recognition.

Key Words: histocompatibility leukocyte antigen class I, splicing defect,truncated heavy chain, melanoma

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