人类白细胞抗原
杂合子丢失
蕈样真菌病
生物
免疫学
淋巴瘤
HLA-B抗原
等位基因
遗传学
抗原
基因
作者
Alexa Kwang,George E. Durán,Sebastian Fernandez‐Pol,Safa Najidh,Shufeng Li,Armando N Bastidas Torres,Erica B. Wang,Melba Herrera,Tarek Bandali,David M. Kurtz,Youn H. Kim,Michael S. Khodadoust
出处
期刊:Blood
[Elsevier BV]
日期:2024-10-10
卷期号:145 (3): 311-324
被引量:3
标识
DOI:10.1182/blood.2024024817
摘要
Abstract Abnormalities involving class I HLA are frequent in many lymphoma subtypes but have not yet been extensively studied in cutaneous T-cell lymphomas (CTCLs). We characterized the occurrence of class I HLA abnormalities in 65 patients with advanced mycosis fungoides or Sézary syndrome. Targeted DNA sequencing, including coverage of HLA loci, revealed at least 1 HLA abnormality in 26 of 65 patients (40%). Twelve unique somatic HLA mutations were identified across 9 patients, and loss of heterozygosity or biallelic loss of HLA was found to affect 24 patients. Although specific HLA alleles were commonly disrupted, these events did not associate with a decrease in the total class I HLA expression. Genetic events preferentially disrupted HLA alleles capable of presenting greater numbers of putative neoantigens. HLA abnormalities co-occurred with other genetic immune evasion events and were associated with worse progression-free survival. Single-cell analyses demonstrated that HLA abnormalities were frequently subclonal. Through analysis of serial samples, we observed that disrupting class I HLA events change dynamically over the disease course. The dynamics of HLA disruption are highlighted in a patient who received pembrolizumab and in whom resistance to pembrolizumab was associated with the elimination of an HLA mutation. Overall, our findings show that genomic class I HLA abnormalities are common in advanced CTCL and may be an important consideration in understanding the effects of immunotherapy in CTCL.
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