4.5 Article

The role of infiltrating lymphocytes in the neo-adjuvant treatment of women with HER2-positive breast cancer

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BREAST CANCER RESEARCH AND TREATMENT
卷 187, 期 3, 页码 635-645

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SPRINGER
DOI: 10.1007/s10549-021-06244-1

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HER2-positive breast cancer; Tumour infiltrating lymphocytes; T-cells; Neo-adjuvant treatment

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资金

  1. Irish Cancer Society's research Centre BreastPredict [CCRC13GAL]
  2. NECRET - the Northeast Cancer Research and Education Trust

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The study found that patients with high levels of lymphocyte counts before treatment were more likely to achieve a complete pathological response after chemotherapy. For patients who achieved a pCR after chemotherapy, their immune response may return to baseline after only one cycle of treatment. In patients who did not achieve a pCR, neoadjuvant treatment may stimulate lymphocyte influx into the tumor.
Background Pre-treatment tumour-associated lymphocytes (TILs) and stromal lymphocytes (SLs) are independent predictive markers of future pathological complete response (pCR) in HER2-positive breast cancer. Whilst studies have correlated baseline lymphocyte levels with subsequent pCR, few have studied the impact of neoadjuvant therapy on the immune environment. Methods We performed TIL analysis and T-cell analysis by IHC on the pretreatment and 'On-treatment' samples from patients recruited on the Phase-II TCHL (NCT01485926) clinical trial. Data were analysed using the Wilcoxon signed-rank test and the Spearman rank correlation. Results In our sample cohort (n = 66), patients who achieved a pCR at surgery, post-chemotherapy, had significantly higher counts of TILs (p = 0.05) but not SLs (p = 0.08) in their pre-treatment tumour samples. Patients who achieved a subsequent pCR after completing neo-adjuvant chemotherapy had significantly higher SLs (p = 9.09 x 10(-3)) but not TILs (p = 0.1) in their 'On-treatment' tumour biopsies. In a small cohort of samples (n = 16), infiltrating lymphocyte counts increased after 1 cycle of neo-adjuvant chemotherapy only in those tumours of patients who did not achieve a subsequent pCR. Finally, reduced CD3 + (p = 0.04, rho = 0.60) and CD4 + (p = 0.01, rho = 0.72) T-cell counts in 'On-treatment' biopsies were associated with decreased residual tumour content post-1 cycle of treatment; the latter being significantly associated with increased likelihood of subsequent pCR (p < 0.01). Conclusions The immune system may be 'primed' prior to neoadjuvant treatment in those patients who subsequently achieve a pCR. In those patients who achieve a pCR, their immune response may return to baseline after only 1 cycle of treatment. However, in those who did not achieve a pCR, neo-adjuvant treatment may stimulate lymphocyte influx into the tumour.

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