Coghill Anna E, Van Bibber Nathan, Baiocchi Robert A, Arnold Susanne M, Riedlinger Gregory, Schneider Bryan P, Zhang Yonghong, Suneja Gita, Gomez Fontela Miguel, Abate-Daga Daniel, Teer Jamie K
Cancer Epidemiology Program, Moffitt Cancer Center, Tampa, Florida.
The Ohio State University Comprehensive Cancer Center, Columbus, Ohio.
Cancer Epidemiol Biomarkers Prev. 2025 May 2;34(5):774-779. doi: 10.1158/1055-9965.EPI-24-1321.
People living with HIV (PWH) have improved life expectancy because of effective human immunodeficiency virus (HIV) therapy but still experience immune impairment (e.g., altered CD4/CD8 T cells). We hypothesized that tumors diagnosed in PWH would have distinct molecular features.
We utilized whole-exome sequencing of paired tumor and germline DNA and RNA from 229 patients with cancer enrolled into the Oncology Research Information Exchange Network to classify total tumor mutation burden (TMB), MHC class I neoantigen count, and MHC class II neoantigen count.
Specimens from 229 patients with cancer (110 PWH and 119 without HIV) were evaluated. Average TMB for tumors diagnosed in PWH was 249, compared with 172 for those without HIV. After adjustment for age, sex, race, smoking, and cancer site, the association between HIV and TMB remained statistically significant (OR = 1.72; 95% confidence interval (CI), 1.26-2.43). We further observed an association between HIV and higher putative class I neoantigen count (OR = 1.62; 95% CI, 1.10-2.41) but no association with putative class II neoantigens. When considering cancer sites separately in unadjusted analyses, average TMB was elevated in PWH for thyroid (P < 0.01) and bladder cancers (P = 0.03) and sarcoma (P = 0.04). Similarly, putative class I neoantigen count was elevated in PWH for head and neck (P < 0.01) and thyroid (P = 0.01) cancers, as well as sarcoma (P = 0.04).
Our findings indicate that tumors diagnosed in PWH harbor a higher TMB and a higher number of putative class I neoantigens.
A higher TMB in PWH may portend a more favorable response to certain cancer treatment modalities such as immune checkpoint inhibitors.
由于有效的人类免疫缺陷病毒(HIV)治疗,HIV感染者(PWH)的预期寿命有所提高,但仍存在免疫功能损害(例如,CD4/CD8 T细胞改变)。我们假设在PWH中诊断出的肿瘤会有独特的分子特征。
我们利用来自肿瘤研究信息交流网络登记的229例癌症患者的配对肿瘤和种系DNA及RNA进行全外显子测序,以分类总肿瘤突变负担(TMB)、MHC I类新抗原计数和MHC II类新抗原计数。
对229例癌症患者(110例PWH和119例无HIV者)的标本进行了评估。PWH中诊断出的肿瘤的平均TMB为249,而无HIV者为172。在调整年龄、性别、种族、吸烟和癌症部位后,HIV与TMB之间的关联仍具有统计学意义(OR = 1.72;95%置信区间(CI),1.26 - 2.43)。我们进一步观察到HIV与较高的推定I类新抗原计数之间存在关联(OR = 1.62;95% CI,1.10 - 2.41),但与推定II类新抗原无关联。在未调整分析中单独考虑癌症部位时,PWH中甲状腺癌(P < 0.01)、膀胱癌(P = 0.03)和肉瘤(P = 0.04)的平均TMB升高。同样,PWH中头颈部癌(P < 0.01)、甲状腺癌(P = 0.01)以及肉瘤(P = 0.04)的推定I类新抗原计数升高。
我们的研究结果表明,PWH中诊断出的肿瘤具有更高的TMB和更多的推定I类新抗原。
PWH中较高的TMB可能预示着对某些癌症治疗方式(如免疫检查点抑制剂)有更良好的反应。
