4.6 Article

Overexpression in metastatic breast cancer supports Syndecan-1 as a marker of invasiveness and poor prognosis

Journal

CLINICAL AND EXPERIMENTAL MEDICINE
Volume 23, Issue 5, Pages 1641-1647

Publisher

SPRINGER-VERLAG ITALIA SRL
DOI: 10.1007/s10238-022-00880-7

Keywords

Syndecan-1 expression; Breast cancer; Brain metastases; Membrane localization; Metastatic process

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Syndecan-1 plays an important role in the metastasis of breast cancer. We observed a shift in cellular localization of syndecan-1, from diffuse cytoplasmic expression in primary breast cancer to membrane expression in metastatic lesions. We also found a correlation between tumor intrinsic subtypes and the extent of syndecan-1 positivity.
Background Metastasis is the main cause of breast cancer (BC) mortality. Increasing evidence points to a role of syndecan-1 (CD138) expression as a prognostic marker involved in BC tissue and leptomeningeal metastasis. Aim of this study was to investigate and compare syndecan-1 tissue expression and localization in primary and secondary BC, focusing on brain metastases. Methods Syndecan-1 expression was determined by immunohistochemistry. Focal vs diffuse (< or > 50% of cancer cells, respectively) pattern of expression, cellular localization (cytoplasm vs membrane) and intensity of immunostaining on neoplastic cells were evaluated. Moreover, the extent and pattern of expression of syndecan-1 were compared between primary tumors and paired metastases and correlated with the tumor intrinsic subtype. Results A total of 23 cases, 10 with paired primary and metastatic tumor and 13 brain metastases, were evaluated. Syndecan-1 was expressed in both primary and metastatic BC. A diffuse cytoplasmic expression was observed in most primary BCs; by contrast, all metastatic lesions showed a membrane pattern of expression, suggesting a shift in cellular localization of syndecan-1 during the metastatic process. Concerning the extent of expression, we observed in metastatic lesions, a trend of association between intrinsic subtypes and extent of positivity. In particular, both BC characterized by overexpression of HER2 and triple-negative tumors were correlated with a diffuse pattern of expression with a moderate to strong intensity. Conclusion A diffuse cytoplasmic expression was observed in most primary BCs; by contrast, all metastatic lesions showed a membrane pattern of expression, suggesting a shift in cellular localization of syndecan-1 during the metastatic process.

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