Department of Public Health Sciences, University of Connecticut Health, Farmington, CT, USA.
Department of Cell Biology, University of Connecticut Health, 263 Farmington Avenue, Farmington, CT, 06030, USA.
Breast Cancer Res Treat. 2024 Nov;208(1):193-200. doi: 10.1007/s10549-024-07455-y. Epub 2024 Sep 4.
Worse survival persists for African-Americans (AA) with breast cancer compared to other race/ethnic groups despite recent improvements for all. Unstudied in outcomes disparities to date is soluble LAG-3 (sLAG-3), cleaved from the LAG-3 immune checkpoint receptor which is a proposed target for deactivation in emerging immunotherapies due to its prominent immunosuppressive function in the tumoral microenvironment. A prior study has found that lower sLAG-3 baseline level was associated with poor outcomes.
In a cross-sectional study of 95 patients with primary breast cancer (n = 58 Caucasian, n = 37 AA), we measured sLAG-3 (ELISA pg/ml) in pre-treatment blood samples using the non-parametric Mann-Whitney u-Test for independent samples, and, calculated Pearson r correlation coefficients of sLAG-3 with circulating cytokines by race.
Mean sLAG-3 level was lower in AA compared to Caucasian patients (1377.6 vs 3690.3, P = .002), and in patients with triple-negative breast cancer (TNBC) compared to those with non-TNBC malignancies (P = .02). When patients with TNBC tumors were excluded from analyses, the difference in sLAG-3 level between AA (n = 21) and Caucasian patients (n = 40) substantially remained (1937.4 vs 4182.4, P = .06). Among Caucasian patients, sLAG-3 was correlated with IL-6, IL-8 and IL-10 (r = .69, P < .001; r = .70, P < .001; and, r = .46, P = .01; respectively). For AA patients, sLAG-3 was correlated only with IL-6 (r = .37, P = .03).
We present the first report that African-American breast cancer patients might have comparatively low pre-treatment sLAG-3 levels, independent of TNBC status, along with reduced co-expression with circulating cytokines. The mechanistic and prognostic role of cleaved LAG-3, particularly in disparate outcomes, remains to be elucidated.
尽管所有种族/族裔群体的近期生存率都有所提高,但与其他种族/族裔群体相比,非裔美国人(AA)的乳腺癌患者的生存率仍然较差。迄今为止,在结局差异方面尚未研究可溶性 LAG-3(sLAG-3),其是 LAG-3 免疫检查点受体的裂解产物,由于其在肿瘤微环境中具有突出的免疫抑制功能,因此被认为是新兴免疫疗法中失活的潜在靶点。先前的研究发现,较低的 sLAG-3 基线水平与不良结局相关。
在一项 95 例原发性乳腺癌患者(n=58 例白种人,n=37 例 AA)的横断面研究中,我们使用非参数 Mann-Whitney u 检验对独立样本中的预处理血液样本中的 sLAG-3(ELISA pg/ml)进行了测量,并计算了 sLAG-3 与种族相关的循环细胞因子的 Pearson r 相关系数。
与白种人患者相比,AA 患者的 sLAG-3 水平较低(1377.6 与 3690.3,P=0.002),并且在三阴性乳腺癌(TNBC)患者中与非 TNBC 恶性肿瘤患者相比(P=0.02)。当从分析中排除 TNBC 肿瘤患者时,AA(n=21)和白种人患者(n=40)之间的 sLAG-3 水平差异仍然很大(1937.4 与 4182.4,P=0.06)。在白种人患者中,sLAG-3 与 IL-6、IL-8 和 IL-10 相关(r=0.69,P<0.001;r=0.70,P<0.001;r=0.46,P=0.01)。对于 AA 患者,sLAG-3 仅与 IL-6 相关(r=0.37,P=0.03)。
我们首次报道,非裔美国乳腺癌患者的术前 sLAG-3 水平可能相对较低,独立于 TNBC 状态,同时与循环细胞因子的表达减少有关。裂解的 LAG-3 的机制和预后作用,特别是在不同结局方面,仍有待阐明。
