Associations between reproductive history, hormone use, APOE epsilon 4 genotype and cognition in middle- to older-aged women from the UK Biobank

L.R.S. Lindseth; A.M.G. de Lange; D. van der Meer; I. Agartz; L.T. Westlye; C.K. Tamnes; C. Barth

doi:10.3389/fnagi.2022.1014605

Associations between reproductive history, hormone use, APOE epsilon 4 genotype and cognition in middle- to older-aged women from the UK Biobank

L.R.S. Lindseth, A.M.G. de Lange, D. van der Meer, I. Agartz, L.T. Westlye, C.K. Tamnes, C. Barth^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

IntroductionRelative to men, women are at a higher risk of developing age-related neurocognitive disorders including Alzheimer's disease. While women's health has historically been understudied, emerging evidence suggests that reproductive life events such as pregnancy and hormone use may influence women's cognition later in life. MethodsWe investigated the associations between reproductive history, exogenous hormone use, apolipoprotein (APOE) epsilon 4 genotype and cognition in 221,124 middle- to older-aged (mean age 56.2 +/- 8.0 years) women from the UK Biobank. Performance on six cognitive tasks was assessed, covering four cognitive domains: episodic visual memory, numeric working memory, processing speed, and executive function. ResultsA longer reproductive span, older age at menopause, older age at first and last birth, and use of hormonal contraceptives were positively associated with cognitive performance later in life. Number of live births, hysterectomy without oophorectomy and use of hormone therapy showed mixed findings, with task-specific positive and negative associations. Effect sizes were generally small (Cohen's d < 0.1). While APOE epsilon 4 genotype was associated with reduced processing speed and executive functioning, in a dose-dependent manner, it did not influence the observed associations between female-specific factors and cognition. DiscussionOur findings support previous evidence of associations between a broad range of female-specific factors and cognition. The positive association between a history of hormonal contraceptive use and cognition later in life showed the largest effect sizes (max. d = 0.1). More research targeting the long-term effects of female-specific factors on cognition and age-related neurocognitive disorders including Alzheimer's disease is crucial for a better understanding of women's brain health and to support women's health care.

Original language	English
Article number	1014605
Number of pages	13
Journal	Frontiers in Aging Neuroscience
Volume	14
Issue number	1
DOIs	https://doi.org/10.3389/fnagi.2022.1014605
Publication status	Published - 19 Jan 2023

Keywords

women's health
cognition
population-based
pregnancy
hormonal contraceptives
hormone therapy
big data
NATURALLY POSTMENOPAUSAL WOMEN
ESTROGEN REPLACEMENT THERAPY
ORAL-CONTRACEPTIVES
SEX-DIFFERENCES
MENOPAUSE
IMPACT
PREGNANCY
MEMORY
PERIOD
RISK

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10.3389/fnagi.2022.1014605Licence: CC BY

Cite this

@article{08dba89acd7d49fea22c251b9445709c,

title = "Associations between reproductive history, hormone use, APOE epsilon 4 genotype and cognition in middle- to older-aged women from the UK Biobank",

abstract = "IntroductionRelative to men, women are at a higher risk of developing age-related neurocognitive disorders including Alzheimer's disease. While women's health has historically been understudied, emerging evidence suggests that reproductive life events such as pregnancy and hormone use may influence women's cognition later in life. MethodsWe investigated the associations between reproductive history, exogenous hormone use, apolipoprotein (APOE) epsilon 4 genotype and cognition in 221,124 middle- to older-aged (mean age 56.2 +/- 8.0 years) women from the UK Biobank. Performance on six cognitive tasks was assessed, covering four cognitive domains: episodic visual memory, numeric working memory, processing speed, and executive function. ResultsA longer reproductive span, older age at menopause, older age at first and last birth, and use of hormonal contraceptives were positively associated with cognitive performance later in life. Number of live births, hysterectomy without oophorectomy and use of hormone therapy showed mixed findings, with task-specific positive and negative associations. Effect sizes were generally small (Cohen's d < 0.1). While APOE epsilon 4 genotype was associated with reduced processing speed and executive functioning, in a dose-dependent manner, it did not influence the observed associations between female-specific factors and cognition. DiscussionOur findings support previous evidence of associations between a broad range of female-specific factors and cognition. The positive association between a history of hormonal contraceptive use and cognition later in life showed the largest effect sizes (max. d = 0.1). More research targeting the long-term effects of female-specific factors on cognition and age-related neurocognitive disorders including Alzheimer's disease is crucial for a better understanding of women's brain health and to support women's health care.",

keywords = "women's health, cognition, population-based, pregnancy, hormonal contraceptives, hormone therapy, big data, NATURALLY POSTMENOPAUSAL WOMEN, ESTROGEN REPLACEMENT THERAPY, ORAL-CONTRACEPTIVES, SEX-DIFFERENCES, MENOPAUSE, IMPACT, PREGNANCY, MEMORY, PERIOD, RISK",

author = "L.R.S. Lindseth and {de Lange}, A.M.G. and {van der Meer}, D. and I. Agartz and L.T. Westlye and C.K. Tamnes and C. Barth",

note = "Funding Information: While working on this study, the authors received funding from the Research Council of Norway (CT: #223273, #288083, #323951; LTW: #273345, #249795, #298646, #300768, #223273; and IA: #213700, #223273, #250358), the South-Eastern Norway Regional Health Authority (CKT: #2019069, #2021070, #500189; LTW: #2018076, #2019101; and IA: #2017097, #2019104, #2020020), the European Research Council under the European Union{\textquoteright}s Horizon 2020 Research and Innovation Program (LTW: #802998), and the Swiss National Science Foundation (A-MGdL: PZ00P3_193658). Funding Information: The work was performed on the Service for Sensitive Data (TSD) platform, owned by the University of Oslo, operated and developed by the TSD service group at the University of Oslo IT-Department (USIT). Publisher Copyright: Copyright {\textcopyright} 2023 Lindseth, de Lange, van der Meer, Agartz, Westlye, Tamnes and Barth.",

year = "2023",

month = jan,

day = "19",

doi = "10.3389/fnagi.2022.1014605",

language = "English",

volume = "14",

journal = "Frontiers in Aging Neuroscience",

issn = "1663-4365",

publisher = "Frontiers Media S.A.",

number = "1",

}

TY - JOUR

T1 - Associations between reproductive history, hormone use, APOE epsilon 4 genotype and cognition in middle- to older-aged women from the UK Biobank

AU - Lindseth, L.R.S.

AU - de Lange, A.M.G.

AU - van der Meer, D.

AU - Agartz, I.

AU - Westlye, L.T.

AU - Tamnes, C.K.

AU - Barth, C.

N1 - Funding Information: While working on this study, the authors received funding from the Research Council of Norway (CT: #223273, #288083, #323951; LTW: #273345, #249795, #298646, #300768, #223273; and IA: #213700, #223273, #250358), the South-Eastern Norway Regional Health Authority (CKT: #2019069, #2021070, #500189; LTW: #2018076, #2019101; and IA: #2017097, #2019104, #2020020), the European Research Council under the European Union’s Horizon 2020 Research and Innovation Program (LTW: #802998), and the Swiss National Science Foundation (A-MGdL: PZ00P3_193658). Funding Information: The work was performed on the Service for Sensitive Data (TSD) platform, owned by the University of Oslo, operated and developed by the TSD service group at the University of Oslo IT-Department (USIT). Publisher Copyright: Copyright © 2023 Lindseth, de Lange, van der Meer, Agartz, Westlye, Tamnes and Barth.

PY - 2023/1/19

Y1 - 2023/1/19

N2 - IntroductionRelative to men, women are at a higher risk of developing age-related neurocognitive disorders including Alzheimer's disease. While women's health has historically been understudied, emerging evidence suggests that reproductive life events such as pregnancy and hormone use may influence women's cognition later in life. MethodsWe investigated the associations between reproductive history, exogenous hormone use, apolipoprotein (APOE) epsilon 4 genotype and cognition in 221,124 middle- to older-aged (mean age 56.2 +/- 8.0 years) women from the UK Biobank. Performance on six cognitive tasks was assessed, covering four cognitive domains: episodic visual memory, numeric working memory, processing speed, and executive function. ResultsA longer reproductive span, older age at menopause, older age at first and last birth, and use of hormonal contraceptives were positively associated with cognitive performance later in life. Number of live births, hysterectomy without oophorectomy and use of hormone therapy showed mixed findings, with task-specific positive and negative associations. Effect sizes were generally small (Cohen's d < 0.1). While APOE epsilon 4 genotype was associated with reduced processing speed and executive functioning, in a dose-dependent manner, it did not influence the observed associations between female-specific factors and cognition. DiscussionOur findings support previous evidence of associations between a broad range of female-specific factors and cognition. The positive association between a history of hormonal contraceptive use and cognition later in life showed the largest effect sizes (max. d = 0.1). More research targeting the long-term effects of female-specific factors on cognition and age-related neurocognitive disorders including Alzheimer's disease is crucial for a better understanding of women's brain health and to support women's health care.

AB - IntroductionRelative to men, women are at a higher risk of developing age-related neurocognitive disorders including Alzheimer's disease. While women's health has historically been understudied, emerging evidence suggests that reproductive life events such as pregnancy and hormone use may influence women's cognition later in life. MethodsWe investigated the associations between reproductive history, exogenous hormone use, apolipoprotein (APOE) epsilon 4 genotype and cognition in 221,124 middle- to older-aged (mean age 56.2 +/- 8.0 years) women from the UK Biobank. Performance on six cognitive tasks was assessed, covering four cognitive domains: episodic visual memory, numeric working memory, processing speed, and executive function. ResultsA longer reproductive span, older age at menopause, older age at first and last birth, and use of hormonal contraceptives were positively associated with cognitive performance later in life. Number of live births, hysterectomy without oophorectomy and use of hormone therapy showed mixed findings, with task-specific positive and negative associations. Effect sizes were generally small (Cohen's d < 0.1). While APOE epsilon 4 genotype was associated with reduced processing speed and executive functioning, in a dose-dependent manner, it did not influence the observed associations between female-specific factors and cognition. DiscussionOur findings support previous evidence of associations between a broad range of female-specific factors and cognition. The positive association between a history of hormonal contraceptive use and cognition later in life showed the largest effect sizes (max. d = 0.1). More research targeting the long-term effects of female-specific factors on cognition and age-related neurocognitive disorders including Alzheimer's disease is crucial for a better understanding of women's brain health and to support women's health care.

KW - women's health

KW - cognition

KW - population-based

KW - pregnancy

KW - hormonal contraceptives

KW - hormone therapy

KW - big data

KW - NATURALLY POSTMENOPAUSAL WOMEN

KW - ESTROGEN REPLACEMENT THERAPY

KW - ORAL-CONTRACEPTIVES

KW - SEX-DIFFERENCES

KW - MENOPAUSE

KW - IMPACT

KW - PREGNANCY

KW - MEMORY

KW - PERIOD

KW - RISK

U2 - 10.3389/fnagi.2022.1014605

DO - 10.3389/fnagi.2022.1014605

M3 - Article

C2 - 36760712

SN - 1663-4365

VL - 14

JO - Frontiers in Aging Neuroscience

JF - Frontiers in Aging Neuroscience

IS - 1

M1 - 1014605

ER -