Peritumoral immune infiltrates in primary tumours are not associated with the presence of axillary lymph node metastasis in breast cancer: a retrospective cohort study

淋巴血管侵犯 乳腺癌 医学 旁侵犯 免疫系统 转移 淋巴结 肿瘤科 腋窝淋巴结 癌症 乳腺癌 内科学 病态的 淋巴系统 病理 免疫学
作者
Carlos López,Ramón Bosch,Guifré Orero,Laia Fontoura Balagueró,Anna Korzyńska,Marcial García‐Rojo,Gloria Bueno,M. Milagro Fernández-Carrobles,Łukasz Roszkowiak,Cristina Callau Casanova,Maria Teresa Salvadó-Usach,Joaquín Jaén Martínez,Albert Gibert‐Ramos,Albert Roso‐Llorach,Andrea Gras Navarro,Marta Berenguer,Montse Llobera,Júlia Gil Garcia,Barbara Tomás,Vanessa Gestí,Eeva Laine,Benoît Plancoulaine,Jordi Baucells,Marylène Lejeune
出处
期刊:PeerJ [PeerJ, Inc.]
卷期号:8: e9779-e9779 被引量:3
标识
DOI:10.7717/peerj.9779
摘要

The axillary lymph nodes (ALNs) in breast cancer patients are the body regions to where tumoral cells most often first disseminate. The tumour immune response is important for breast cancer patient outcome, and some studies have evaluated its involvement in ALN metastasis development. Most studies have focused on the intratumoral immune response, but very few have evaluated the peritumoral immune response. The aim of the present article is to evaluate the immune infiltrates of the peritumoral area and their association with the presence of ALN metastases.The concentration of 11 immune markers in the peritumoral areas was studied in 149 patients diagnosed with invasive breast carcinoma of no special type (half of whom had ALN metastasis at diagnosis) using tissue microarrays, immunohistochemistry and digital image analysis procedures. The differences in the concentration of the immune response of peritumoral areas between patients diagnosed with and without metastasis in their ALNs were evaluated. A multivariate logistic regression model was developed to identify the clinical-pathological variables and the peritumoral immune markers independently associated with having or not having ALN metastases at diagnosis.No statistically significant differences were found in the concentrations of the 11 immune markers between patients diagnosed with or without ALN metastases. Patients with metastases in their ALNs had a higher histological grade, more lymphovascular and perineural invasion and larger-diameter tumours. The multivariate analysis, after validation by bootstrap simulation, revealed that only tumour diameter (OR = 1.04; 95% CI [1.00-1.07]; p = 0.026), lymphovascular invasion (OR = 25.42; 95% CI [9.57-67.55]; p < 0.001) and histological grades 2 (OR = 3.84; 95% CI [1.11-13.28]; p = 0.033) and 3 (OR = 5.18; 95% CI [1.40-19.17]; p = 0.014) were associated with the presence of ALN metastases at diagnosis. This study is one of the first to study the association of the peritumoral immune response with ALN metastasis. We did not find any association of peritumoral immune infiltrates with the presence of ALN metastasis. Nevertheless, this does not rule out the possibility that other peritumoral immune populations are associated with ALN metastasis. This matter needs to be examined in greater depth, broadening the types of peritumoral immune cells studied, and including new peritumoral areas, such as the germinal centres of the peritumoral tertiary lymphoid structures found in extensively infiltrated neoplastic lesions.
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