1. Radiation-Related Deregulation of TUBB3 and BRCA1/2 and Risk of Secondary Lung Cancer in Women With Breast Cancer
- Author
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Vincenzo Fontana, Carlo Genova, Alberto Ballestrero, G. Burrafato, Francesco Grossi, Erika Rijavec, Claudio Sini, Angela Alama, Simona Coco, Silvia Bonfiglio, Sandra Salvi, Luca Longo, Maria Giovanna Dal Bello, Franca Carli, Giulia Barletta, Simona Boccardo, Zita Cavalieri, Marco Mora, Federica Biello, and Irene Vanni
- Subjects
Adult ,0301 basic medicine ,Oncology ,Cancer Research ,medicine.medical_specialty ,Lung cancer risk ,Lung Neoplasms ,DNA Repair ,medicine.medical_treatment ,Estrogen receptor ,Breast Neoplasms ,DNA-repair pathway ,03 medical and health sciences ,0302 clinical medicine ,Breast cancer ,Tubulin ,Internal medicine ,medicine ,Humans ,skin and connective tissue diseases ,Lung cancer ,Hormonal asset ,BRCA2 Protein ,BRCA1 Protein ,business.industry ,Cancer ,Middle Aged ,medicine.disease ,DNA-Binding Proteins ,Radiation therapy ,030104 developmental biology ,BRCA1/2 compensatory effect ,Case-Control Studies ,030220 oncology & carcinogenesis ,Concomitant ,Immunohistochemistry ,Female ,Secondary unrelated cancer ,ERCC1 ,business - Abstract
Introduction Breast cancer survivors are at increased risk of developing unrelated primary cancers, particularly lung cancer. Evidence indicates that sex hormones as well as a deregulation of DNA-repair pathways may contribute to lung cancer onset. We investigated whether the hormone status and expression of markers involved in DNA repair (BRCA1/2, ERCC1, and P53R2), synthesis (TS and RRM1), and cell division (TUBB3) might be linked to lung cancer risk. Patients and Methods Thirty-seven breast cancer survivors with unrelated lung cancer and 84 control subjects comprising women with breast cancer (42/84) or lung cancer (42/84) were enrolled. Immunohistochemistry on tumor tissue was performed. Geometric mean ratio was used to assess the association of marker levels with patient groups. Results Estrogen receptor was expressed in approximately 90% of the breast cancer group but was negative in the majority of the lung cancer group, a result similar to the lung cancer control group. Likewise, ER isoform β was weakly expressed in the lung cancer group. Protein analysis of breast cancer versus control had a significantly lower expression of BRCA1, P53R2, and TUBB3. Likewise, a BRCA1 reduction was observed in the lung cancer group concomitant with a BRCA2 increase. Furthermore, BRCA2 and TUBB3 increased in ipsilateral lung cancer in women who had previously received radiotherapy for breast cancer. Conclusion The decrease of DNA-repair proteins in breast cancer could make these women more susceptible to therapy-related cancer. The increase of BRCA2 and TUBB3 in lung cancer from patients who previously received radiotherapy for breast cancer might reflect a tissue response to exposure to ionizing radiation.
- Published
- 2020