PO.CL09.04 · 临床研究

Population analysis and immunologic landscape of melanoma in people living with HIV

编号 7862 展板 14 时间 4/22 09:00–12:00 区域 Section 46 主讲 Gabriele Romano, BS;MS;PhD
分会场 Real World Impact of Prognostic and Predictive Parameters
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作者与单位

Lindsay Barger1, Derek Wang2, Ashley Saravia1, Valeria Mezzano-Robinson3, Gyles Ward3, Cynthia Loomis3, Carly Feldman4, Madalina Tuluc4, Rino S. Seedor4, Peter J. Gaskill1, Anna E. Coghill5, Gita Suneja6, Iman Dehzangi2, Jenna Hope1, George Jour3, Gabriele Romano1

1Drexel University College of Medicine, Philadelphia, PA,2Rutgers University, Camden, NJ,3NYU Langone Health, New York, NY,4Thomas Jefferson University, Philadelphia, PA,5Moffitt Cancer Center, Tampa, FL,6Huntsman Cancer Institute, Salt Lake City, UT

摘要 Abstract

Purpose: To dissect the clinical and immunological features of people living with HIV (PLWH) diagnosed with melanoma, who have consistently shown worse outcomes than HIV-negative individuals (PLw/oH) with the same cancer. Experimental Design: We analyzed electronic health records from 1,087 PLWH and 394,437 PLw/oH with melanoma. Demographic and clinical characteristics were compared. Spatial immune transcriptomics (72 immune-related genes) was performed on melanoma tumor samples (n=11), with downstream validation using multiplex immunofluorescence (n=15 PLWH, n=14 PLw/oH). Results: PLWH were diagnosed at a younger age, had greater representation of Hispanic and Black individuals, and showed reduced survival. They also had a markedly increased risk of brain metastases. PLWH experienced significant delays in initiating immune checkpoint inhibitor (ICI) therapy and had worse post-ICI survival, even after balancing covariates. Spatial transcriptomics revealed a more immunosuppressive tumor microenvironment in PLWH, with increased transcription of immune checkpoints (PD1, LAG3) and reduced antigen-presentation markers (HLA-DRB, B2M), with distinct spatial distributions in tumors and surrounding microenvironments. Multiplex immunofluorescence demonstrated features of an exhausted CD8⁺ T cell compartment, including enrichment of PD1 int LAG3⁻ and PD1 int LAG3⁺ subpopulations, and a significant accumulation of myeloid-derived suppressor cells (CD11b⁺ HLA-DR⁻ CD33⁺). Conclusions: Melanoma in PLWH is associated with distinct clinical and immunological features, including delayed ICI treatment, reduced survival, and an immunosuppressive microenvironment with exhausted CD8⁺ T cells and expanded myeloid-derived suppressor cells. These findings suggest that chronic HIV infection may impair antitumor immunity in melanoma. Targeting the pathways identified here may improve therapeutic responses and outcomes in this population.
利益披露 Disclosure
L. Barger, None.. D. Wang, None.. A. Saravia, None.. V. Mezzano-Robinson, None.. G. Ward, None.. C. Loomis, None.. C. Feldman, None.. M. Tuluc, None.. R. S. Seedor, None.. P. J. Gaskill, None.. G. Suneja, None.. I. Dehzangi, None.. J. Hope, None.. G. Jour, None.. G. Romano, None.

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