The Impact of APOE and Smoking History on Cognitive Function in Older, Long-term Breast Cancer Survivors

Overview

Journal J Cancer Surviv

Specialty Oncology

Date 2022 Oct 24

PMID 36279076

Authors

Tim A Ahles

Irene Orlow

Elizabeth Schofield

Yuelin Li

Elizabeth Ryan

James C Root

Sunita K Patel

Katrazyna McNeal

Alexandra Gaynor

Heidi Tan

Vani Katheria

Jessica Vazquez

Sergio Corrales-Guerrero

Keimya Sadeghi

Tiffany Traina

Arti Hurria

Affiliations

Soon will be listed here.

Abstract

Purpose: This study aims to determine whether older breast cancer survivors score lower on neuropsychological tests compared to matched non-cancer controls and to test the hypotheses that survivors who were APOE ε4 carriers would have the lowest cognitive performance but that smoking history would decrease the negative effect of ε4 on cognition.

Methods: Female breast cancer survivors who had been diagnosed and treated at age 60 or older and were 5-15-year survivors (N = 328) and age and education matched non-cancer controls (N = 162) were assessed at enrollment and at 8-, 16-, and 24-month follow-ups with standard neuropsychological and psychological assessments. Blood for APOE genotyping was collected, and smoking history was assessed at enrollment. Participants were purposely recruited so that approximately 50% had a history of treatment with chemotherapy or no chemotherapy and approximately 50% had a smoking history.

Results: After adjusting for age, cognitive reserve, depression, and fatigue, breast cancer survivors scored significantly lower on all domains of cognitive function. A significant two-way interaction demonstrated that the negative effect of ε4 on cognitive performance was stronger among survivors. A significant three-way interaction supported the hypothesis that smoking history had a protective effect on cognitive function in ε4 carriers that was more pronounced in the controls than the survivors.

Conclusions: The results support the long-term cognitive impact of breast cancer diagnosis and treatments on older, disease-free survivors, particularly for ε4 carriers. The results also emphasize the importance of assessing smoking history when examining APOE and cognition and are an example of the complex interactions of age, genetics, health behaviors, and disease history in determining cognitive function.

Implications For Cancer Survivors: These results help explain why only a subset of breast cancer survivors appear to be vulnerable to cognitive problems.

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