Posttraumatic Stress Disorder Symptoms and Cardiovascular and Brain Health in Women

Key Points

Question 
Are posttraumatic stress disorder (PTSD) symptoms associated with poorer cardiovascular and neurocognitive health among midlife women, and do these associations vary by APOEε4 status?

Findings 
In this cross-sectional study of 274 midlife women, women with higher PTSD symptoms had significantly greater carotid atherosclerosis. Among women who were carriers of the APOEε4 genotype, those with higher PTSD symptoms had greater brain white matter hyperintensities, an indicator of brain small vessel disease, as well as poorer cognition.

Meaning 
These findings suggest that adverse implications of PTSD symptoms for both cardiovascular and neurocognitive health at midlife, particularly for women who are carriers of APOEε4.

Importance 
Posttraumatic stress disorder (PTSD), cardiovascular disease (CVD), and Alzheimer disease are major public health issues, particularly for women. The implications of PTSD for cardiovascular and brain health for women is poorly understood.

Objective 
To assess whether PTSD symptoms among midlife women are associated with carotid intima media thickness (IMT), an indicator of carotid atherosclerosis; brain white matter hyperintensity volume (WMHV), an indicator of brain small vessel disease; and cognitive performance and to test a modifying role of the APOEε4 genotype.

Design, Setting, and Participants 
In this cross-sectional study, participants were enrolled between 2016 to 2021 and completed questionnaires (PTSD Checklist–Civilian Version), physical measures, phlebotomy, neuropsychological testing, a carotid ultrasonographic examination, and 3-Tesla brain magnetic resonance imaging. Participants included community-based women ages 45 to 67 years without a history of CVD, stroke, or dementia. Data were analyzed from July 2022 to September 2023.

Exposures 
PTSD symptoms.

Main Outcomes and Measures 
Outcomes of interest were associations of PTSD symptoms with carotid IMT, brain WMHV, and cognition, assessed in linear regression models. Interactions by APOEε4 were tested. Covariates included age, race and ethnicity, education, and CVD risk factors.

Results 
Among 274 participants (mean [SD] age, 59.03 [4.34] years; 6 Asian participants [2.2%]; 48 Black participants [17.5%]; 215 White participants [78.5%]; 5 multiracial participants [1.8%]), 64 participants (24.71%) were APOEε4 genotype carriers. Higher PTSD symptoms were associated with greater carotid IMT (multivariable β = 0.07 [95% CI, 0.01 to 0.13]; P = .03). Associations of PTSD symptoms with neurocognitive outcomes significantly varied by APOEε4 status. Among women with APOEε4, PTSD symptoms were associated with greater whole-brain WMHV (β = 0.96 [95% CI, 0.30 to 1.63]; P = .009), periventricular WMHV (β = 0.90 [95% CI, 0.24 to 1.56]; P = .02), deep WMHV (β = 1.21 [95% CI, 0.23 to 2.20]; P = .01), and frontal WMHV (β = 1.25 [95% CI, 0.05 to 2.45]; P = .04), as well as with poorer cognition, specifically attention and working memory (β = −3.37 [95% CI, −6.12 to −0.62]; P = .02), semantic fluency (β = −6.01 [95% CI, −10.70 to −1.31]; P = .01), perceptual speed (β = −12.73 [95% CI, −20.71 to −4.75]; P = .002), and processing speed (β = −11.05 [95% CI, −17.80 to −4.30]; P = .002) in multivariable models.

Conclusions and Relevance 
In this cross-sectional study of midlife women, greater PTSD symptoms were associated with higher carotid atherosclerosis and, among women who were APOEε4 carriers, greater brain small vessel disease and poorer cognitive performance. These findings point to the adverse implications of PTSD symptoms for cardiovascular and neurocognitive health among women in midlife, particularly for women who are APOEε4 carriers.

Introduction

Cardiovascular disease (CVD) and Alzheimer disease (AD) are major women’s health issues. CVD is the leading cause of death among US women, with 45% of women developing CVD in their lifetime.1 AD is the fourth leading cause of death among US women.2 Furthermore, approximately two-thirds of individuals with AD and related disorders are women.3

An issue with relevance for cardiovascular and neurocognitive health is posttraumatic stress disorder (PTSD). Most women in the US will experience at least 1 major traumatic event in their life,4 and 10% will develop PTSD. Women have double the risk of PTSD relative to men.5 PTSD is associated with a 50% to 60% increased risk of incident CVD6 and elevated stroke7 and dementia8 risk.

While evolving literature links PTSD to women’s cardiovascular and neurocognitive health, key questions remain. First, the existing literature relies on male samples, with few studies in women and even fewer among midlife women. An exception is the Nurses’ Health Study II (NHS II) of midlife women, which found associations between increased PTSD symptoms and worse cognitive function assessed via a self-administered online cognitive battery.9-11 However, NHS II lacked vascular and brain health measures. Midlife is a critical time for women’s cardiovascular and brain health, as it occurs directly before the onset of clinical CVD12 and is when initial hallmarks of AD and related disorders (eg, amyloid β, hyperphosphorylated tau) begin.13 Midlife includes menopause, a time of accelerating vascular risk,14 decreased memory,15 and potential emergence of effects of earlier stress exposure.16 Second, although the interconnections between the heart and the brain are increasingly appreciated,17 few studies bridge these systems. Furthermore, few studies have considered a role for the APOEε4 (OMIM 107741) genotype, a risk factor for poor cardiovascular health, cognitive decline, and dementia, particularly for women, and potentially pointing to women particularly vulnerable to neurocognitive and cardiovascular insults.18,19

We tested whether higher PTSD symptoms would be associated with higher carotid IMT, greater brain white matter hyperintensity (WMH) or volume (WMHV), and poorer cognition among midlife women who underwent vascular imaging, neuroimaging, and a comprehensive neuropsychological battery. Carotid IMT, or ultrasonographically assessed thickness of the intimal and medial layers of the carotid artery, is an established subclinical CVD indicator associated with future CVD events and useful for assessing cardiovascular health among midlife women among whom other subclinical indicators (eg, coronary calcification) may lack sensitivity.20,21 WMHs are lesions in the white matter apparent on magnetic resonance imaging (MRI) that reflect, in part, small vessel disease and are linked to later dementia, cognitive decline, and mortality.22 Collectively, IMT and WMHs help identify women at risk for future disease. Furthermore, we tested a modifying role of the APOEε4 genotype, hypothesizing that women who were APOEε4 carriers would be at particularly elevated cardiovascular and neurocognitive risk with PTSD symptoms.

This cross-sectional study was reviewed and approved by the University of Pittsburgh Human Research Protection Office. Participants provided written informed consent. This study follows the Strengthening the Reporting of Observational Studies in Epidemiology (STROBE) reporting guideline for cross-sectional studies. Participants underwent screening procedures, physical measurements, medical history interview, questionnaires, phlebotomy, neuropsychological testing, carotid artery ultrasonography, and brain MRI.

The MsBrain study included 274 women ages 45 to 67 years recruited in 2017 to 2020 for a study of menopause and brain health.23 Participants were recruited from the Pittsburgh, Pennsylvania, community via advertisements, registry mailings, and a menopause and cardiovascular health study.24 MsBrain exclusion criteria reflected the parent study on menopause and included pregnancy, hysterectomy or bilateral oophorectomy, history of stroke or cerebrovascular accident, Parkinson disease, current chemotherapy, history of dementia, seizure disorder, brain tumor, active substance abuse (established via urine toxicology screen), history of head trauma with loss of consciousness more than 60 minutes, contraindication to MRI, and use of systemic estrogen or progesterone, selective estrogen receptor modulators, aromatase inhibitors, gabapentin, selective serotonin reuptake inhibitors, or serotonin norepinephrine reuptake inhibitors.

Of 664 women screened, 274 women were eligible, enrolled, and underwent study procedures. The number of women in models varied by the outcome under study (IMT, WMHV, cognition). For IMT, 272 women underwent a carotid ultrasonographic examination, and since 2 women were missing phlebotomy, 270 women were included in models with blood biomarkers. For WMHV, 239 women underwent neuroimaging, 9 were excluded due to brain tumor, stroke, or seizure disorder detected, and 5 women were excluded due to a chemotherapy history, yielding 225 women included in analyses (223 women with blood biomarkers). For cognition, 9 women were excluded due to brain tumor, stroke, or seizure disorder, 1 woman was excluded due to tardive dyskinesia, and 8 women were excluded from select tests due to English language limitations, yielding 261 included in analyses. Finally, due to refusal of genetic testing, analyses incorporating APOE included 257 women for IMT, 215 women for WMHV, and 247 women for cognition. Women excluded from any model had a higher body mass index (BMI; calculated as weight in kilograms divided by height in meters squared) (31.25 vs 28.21; t272 = 2.9; P = .004) and were more likely to be Black (35.94% vs 11.90%; Cramer V = 0.26; P < .001) than women included in all models.

PTSD Symptoms

The PTSD Checklist–Civilian Version (PCL-C)25 is a validated, 17-item self-report inventory assessing PTSD symptoms over the past month, with items rated from 1, indicating not at all, to 5, extremely, and higher scores indicating higher PTSD symptoms. Primary models considered the continuous summed score and secondary models categorized PTSD by the clinical cutoff (≥30).26,27

Carotid Ultrasonography

Certified sonographers at the University of Pittsburgh’s Ultrasound Research Laboratory obtained bilateral carotid images via B-mode ultrasonography using a Sonoline Antares (Siemens) high-resolution duplex scanner (VF10-5 transducer) according to a standardized protocol.28 Digitized images were obtained at end-diastole from 8 locations (4 locations from left and right carotid arteries): near and far walls of the distal common carotid artery, far walls of the carotid bulb, and the internal carotid artery. Images were read using semiautomated reading software. Values were obtained by electronically tracing the lumen-intima interface and the media-adventitia interface across a 1-cm segment for each segment. IMT was the mean of the mean readings across the 8 locations. Reproducibility was excellent (intraclass correlation coefficient: between sonographers, ≥0.87; between readers, 0.92).

MRI scanning was performed at the MR Research Center of the University of Pittsburgh with a 3T Siemens Tim Trio MR scanner and a Siemens 64-channel head coil.23 MRIs were magnetization-prepared rapid gradient echo (MPRAGE) T1-weighted sequence and T2-weighted (T2w) fluid-attenuated inversion recovery (FLAIR) sequence. MPRAGE images were acquired in the axial plane (parameters: repetition time, 2400 ms; echo time, 2.22 ms; T1, 1000 ms; flip angle, 8°; field of view, 256 × 240 mm; slice thickness, 0.8 mm; voxel size, 0.8 mm × 0.8mm; matrix size, 320 × 300; number of slices, 208). FLAIR images were acquired in the axial plane (parameters: repetition time, 9690 or 10 000 ms; echo time, 91 ms; T1, 2500 ms; flip angle, 135°; field of view, 256 × 256 mm; matrix, 320 × 320; slice thickness, 1.6 mm; voxel size, 0.8 mm × 0.8 mm; number of slices, 104).

An automated pipeline was used to segment WMH on the T2w FLAIR images using previously validated methods.29 Cerebral and cerebellar white matter were segmented on the T1w image and mapped into the T2w FLAIR image space using SPM mapping software version 12 (Functional Imaging Laboratory, UCL Queen Square Institute of Neurology) and FreeSurfer processing, analyzing, and visualizing software version 7.1.1 (Athinoula A. Martinos Center for Biomedical Imaging, Harvard Medical School). Cerebellar white matter represented normal-appearing white matter; its intensity mean and SD were used for Z-transformation of the T2w FLAIR image. A threshold of 2 was applied on Z-transformed FLAIR images. Z-transformation also reduces intensity variations across individual FLAIR images.

In the processing, analyzing, and visualizing software, white matter was parcellated according to its nearest cortex with the Deskian-Killiany atlas, used to generate the cortical white matter masks for frontal, temporal, parietal, and occipital lobes for localization of WMHs. White matter parcellations corresponding to frontal cortex regions were combined to create a frontal cortical white matter mask to localize frontal WMHs. Cortical white matter masks were generated for temporal, parietal, and occipital lobes. These lobular cortical white matter masks did not overlap and were combined to create an overall cortical and deep white matter mask. White matter surrounding the ventricles that was not part of the cortical and deep white matter mask comprised the periventricular white matter mask. The total and regional WMHV (in centimeters cubed) were normalized as WMH divided by intracranial volume and log transformed.

Cognitive Performance

Trained and certified testers administered an in-person neuropsychological battery. Participants were tested for attention and working memory using the Letter-Number Sequencing,30 control and experimental versions. Processing speed was tested using the Symbol Digit Modalities Test.31 Participant perceptual speed was tested using Finding A’s.32 Memory was assessed using the California Verbal Learning Test-233 short and long-delay free recall, and learning was tested using the California Verbal Learning Test-2 total score on trials 1 to 5. We assessed letter fluency using the Letter Fluency Test PRW set.34 Semantic fluency was assessed with the animals task.35 Spatial ability was assessed with the Card Rotations Test.32 Finally, global cognitive function was assessed with the Montreal Cognitive Assessment.36

Additional Measures

Height and weight were measured via standard methods and BMI was calculated. Systolic blood pressure (SBP) and diastolic blood pressure (DBP) were the mean of 3 seated measurements. Demographics, medical history, and medication use were assessed by questionnaires and interview. Race, ethnicity, gender, and education (years of education) were self-reported. Race and ethnicity were assessed because due to previously documented differences in PTSD, cardiovascular, and neurocognitive risk. Race and ethnicity were categorized as Asian, Black, White, or multiracial. Head injury history was assessed. Current and lifetime substance use (eg, amphetamines, opiates, hallucinogens, benzodiazepines, marijuana) was assessed via urine toxicology screen and questionnaire. Physical activity was assessed using the International Physical Activity Questionnaire,37 and depressive symptoms were assessed with the Center for Epidemiologic Studies of Depression scale.38

Women underwent phlebotomy after overnight fast. Glucose, total cholesterol, high density lipoprotein (HDL) cholesterol, and triglycerides were determined using enzymatic assays and insulin via immunoturbidimetric assay. Low-density lipoprotein (LDL) cholesterol was calculated via the Friedewald equation.39 Homeostatic model assessment (HOMA) for insulin resistance was calculated as (insulin × glucose) / 22.5. Genotypes for APOE polymorphisms, rs429358 (APOEε4), and rs7412 (APOEε2) were determined using TaqMan genotyping assays (Thermo Fisher Scientific).40 Because of the strong linkage disequilibrium between sites, this is also treated as a 3-allele APOE polymorphism: APOEε2, APOEε3, and APOEε4, yielding 6 genotypes (ε2/ε2, ε2/ε3, ε2/ε4, ε3/ε3, ε3/ε4, ε4/ε4). Participants were classified as APOEε4 carriers (ε2/ε4, ε3/ε4, ε4/ε4) or not (ε2/ε2, ε2/ε3, ε3/ε3).

Statistical Analysis

PTSD symptoms, IMT, BMI, HOMA, triglycerides, physical activity, and WMHV were log transformed. We tested our primary aims in separate linear regression models testing associations of PTSD symptoms with IMT, PTSD symptoms with whole-brain WMHV, and PTSD symptoms with cognitive performance. Regional WMHV were considered secondarily. Covariates in models of IMT or WMHV were age, race and ethnicity, education, BMI, SBP, HOMA, HDL, triglycerides, smoking, physical activity, and use of BP-lowering, diabetes, and lipid medications. While covariates were selected in an a priori manner, 1 BP variable (SBP) and HDL and triglycerides were included in models, given collinearity between BP variables and between lipid variables, respectively. Covariates for models of cognitive performance were age, race and ethnicity, and education. Interactions between PTSD and APOEε4 in relation to study outcomes (IMT, WMH, cognition) were tested in separate models; where there was a significant interaction, models were stratified by APOEε4 status. Given the number of cognitive tests administered, in additional cognitive outcome models, we used the false discovery rate method to account for multiple comparisons.41 In sensitivity analyses, we considered associations of PTSD with IMT, WMH, or cognition also covarying for substance use, head injury history, or depressive symptoms (given the high correlation between depressive and PTSD symptoms [r = 0.67], a residualized depressive symptom score was considered). In additional secondary models, we tested an indirect effect of IMT in the association of PTSD symptoms with WMHV or cognition via Sobel tests. We similarly considered an indirect effect of WMHV in associations of PTSD symptoms with cognition in separate models. For all models, diagnostic statistics and graphical outputs were examined to assess model assumptions, model fit, and influence of individual data points. Tests were 2-tailed with α = .05. Analyses were conducted in SAS software version 9.4 (SAS Institute). Data were analyzed from July 2022 to September 2023.

Among 274 participants (mean [SD] age, 59.03 [4.34] years; 6 Asian participants [2.2%]; 48 Black participants [17.5%]; 215 White participants [78.5%]; 5 multiracial participants [1.8%]), 64 participants (24.71%) were APOEε4 genotype carriers. Participants had a median (IQR) BMI of 27.36 (23.99-32.68), and mean (SD) SBP was 118.93 (15.06) mm Hg and DBP was 68.52 (8.90) mm Hg (Table 1).

We first examined the IMT. Women with greater PTSD symptoms had higher carotid IMT (Table 2), and associations persisted controlling for CVD risk factors. Associations between PTSD and IMT did not significantly vary by APOEε4 status (P for interaction = .71).

In the WMHV models, interactions between PTSD symptoms and APOEε4 status were observed in the primary outcome of whole-brain WMHV (P for interaction = .02), as well as periventricular (P for interaction = .03) and parietal WMHV (P for interaction = .03) in multivariable models. Among women who were APOEε4 carriers, PTSD symptoms were associated with greater whole-brain (β = 0.96 [95% CI, 0.30 to 1.63]; P = .009), periventricular (β = 0.90 [95% CI, 0.24 to 1.56]; P = .02), deep (β = 1.21 [95% CI, 0.23 to 2.20]; P = .01), and frontal (β = 1.25 [95% CI, 0.05 to 2.45]; P = .04) WMHV (Table 3 and Figure 1).

We observed significant interactions between PTSD symptoms and APOEε4 status in association with cognitive outcomes, specifically attention and working memory, semantic fluency, processing speed, and perceptual speed. Among women who were APOEε4 carriers, PTSD symptoms were associated with poorer attention and working memory (β = −3.37 [95% CI, −6.12 to −0.62]; P = .02), semantic fluency (β = −6.01 [95% CI, −10.70 to −1.31]; P = .01), processing speed (β = −11.05 [95% CI, −17.80 to −4.30]; P = .002), and perceptual speed (β = −12.73 [95% CI, −20.71 to −4.75]; P = .002) (Figure 2; eTable 1 in Supplement 1).

In secondary models, given the number of neuropsychological tests considered, associations between PTSD and cognition were tested controlling for multiple comparisons. Findings for processing speed and perceptual speed remained among women who were APOEε4 carriers (eTable 1 in Supplement 1). We also considered associations of PTSD with outcomes using the PCL-C clinical cutoff; 51 women (19%) scored in this range. Whereas clinically elevated PTSD symptoms were not significantly associated with IMT, among women who were APOEε4 carriers, PTSD symptoms were associated with higher whole-brain WMHV, deep WMHV, and poorer processing speed and perceptual speed (eTables 2-4 in Supplement 1). Furthermore, additionally covarying for depressive symptoms, history of head injury, or substance use history did not account for associations of PTSD with IMT, WMHV, or cognition (eTables 5-7 in Supplement 1). Finally, there was no evidence of an indirect effect of IMT in associations between PTSD and WMHV (whole-brain WMHV: β = 0.12 [95% CI, −0.10 to 0.35]; P = .29), nor any indirect effects of IMT (eg, processing speed: β = 0.20 [95% CI, −0.76 to 1.16]; P = .68) or whole-brain WMHV (eg, processing speed: β = 0.07 [95% CI, −2.92 to 3.06]; P = .96) in associations of PTSD with cognitive performance among women who were APOEε4 carriers.

Discussion

In this cross-sectional study among midlife women, higher PTSD symptoms were associated with greater carotid atherosclerosis. Furthermore, among women who were APOEε4 carriers, PTSD symptoms were associated with greater WMHV (whole brain, periventricular, deep, frontal) and poorer cognitive performance across multiple domains. These findings point to the adverse outcomes associated with PTSD symptoms for cardiovascular and neurocognitive health at midlife, particularly for women who are APOEε4 carriers.

Some prior studies, largely focused on men and/or veterans, have considered PTSD symptoms in relation to cardiovascular or brain health. For IMT, some studies have reported that PTSD is associated with higher IMT, yet findings are mixed and focused on male veterans or specific populations (eg, adults experiencing deportation).42,43 Some studies have indicated associations of PTSD symptoms with WMH44 and cognition,45 yet these studies relied on data from males, veterans, and/or individuals undergoing PTSD treatment. The NHS II of midlife women found that women with histories of trauma exposure and more PTSD symptoms had greater declines in cognitive performance over approximately 1 year compared with women without PTSD symptoms.10 However, in the NHS II study, cognitive performance was assessed via a brief online battery assessing 2 domains: learning and working memory and psychomotor speed and attention. Our study is notable for its assessment of cognition via a comprehensive, in-person neuropsychological test battery assessing a range of domains. Collectively, this study underscores the sensitivity of working memory, psychomotor speed, and perceptual speed and visual attention to PTSD symptoms. MsBrain also shows the importance of APOEε4 genotype status in these associations. Thus, this study sheds important insight on the implications of PTSD symptoms to women’s cardiovascular and neurocognitive health.

Our study is notable in considering the APOEε4 genotype, which is associated with dementia risk, particularly in women.18 Prior studies have also found that the APOEε4 genotype is associated with elevated CVD and PTSD risk,19,46,47 and studies with male veterans considered APOEε4 in associations of PTSD to cognition.48,49 In our study, APOEε4 genotype was an important modifier of associations of PTSD with neurocognitive outcomes but not carotid atherosclerosis, perhaps due to the greater potency of the APOEε4 genotype in neurocognitive risk.18 Our findings indicate that the APOEε4 genotype may identify a group of women with PTSD symptoms at particular risk for poor neurocognitive health.

We considered PTSD symptoms in association with the regional distribution of WMHV. Women who were APOEε4 carriers who had higher PTSD symptoms had greater whole-brain WMHV, periventricular WMHV, deep WMHV, and WMHV in the frontal lobe. Notably, frontal lobe WMHs have been particularly linked to vascular risk,50 suggesting the importance of vascular processes here.

The potential mechanisms linking PTSD symptoms to cardiovascular and neurocognitive health are multiple. PTSD has been associated with poorer CVD risk factors, which contribute to the development of vascular disease,51 yet we controlled for these factors. We considered education, depressive symptoms, head injury, and substance use, which did not explain associations. PTSD symptoms have been associated with altered emotion processing and neural circuitry implicated in cognition45 and stressor-induced cardiovascular reactivity.52 Other potential pathways, such as inflammatory, autonomic, hypothalamic pituitary adrenal, or epigenetic processes, warrant future consideration.

This study has several strengths. It included a large, well-characterized community sample of midlife women. It leveraged vascular and neuroimaging, providing subclinical indicators of peripheral vascular and cerebrovascular health decades before clinical disease is present. A comprehensive neuropsychological battery was performed. APOE genotyping was conducted, showing pronounced modification by APOEε4 status. The interconnections between the cardiovascular system and brain are increasingly appreciated; this study is unique in considering them together, showing implications of PTSD across systems.

Limitations

This study has some limitations. We did not conduct diagnostic clinical interviews, nor did we assess PTSD treatment. Study exclusions included common antidepressants, head injury, active substance use, and several cardiovascular and neurological diseases. Thus, participants were likely less distressed and healthier than the general population, which may have restricted the range on certain indicators. Participants had relatively low levels of PTSD symptoms, yet it is notable that associations were observed even at these low levels. To measure PTSD symptoms, we used the PCL-C, based on Diagnostic and Statistical Manual of Mental Disorders (Fourth Edition) PTSD criteria, rather than measures (eg, PCL-5) based on Diagnostic and Statistical Manual of Mental Disorders (Fifth Edition) criteria. However, there is high agreement between PCL-C and PCL-5.53 Women excluded from any model had a higher BMI and were more often Black than women included in all models. Furthermore, all participants identified as cisgender, and most were non-Hispanic Black or White. Results may not generalize to all groups. Future work should consider more diverse samples. Given the multiple tests conducted, results, particularly for secondary findings, should be regarded with caution. The study was observational and cross-sectional; we cannot make assertions about directionality or causality.

Conclusions

The findings of this cross-sectional study underscore the important implications of PTSD and its symptoms for women’s cardiovascular and brain health, with women who were APOEε4 carriers particularly at risk. PTSD is a major women’s health issue, affecting 10% of women in their lifetime. Our findings point to an at-risk population that may warrant early intervention and prevention efforts to reduce cardiovascular and neurocognitive risk at midlife and beyond.

Accepted for Publication: September 23, 2023.

Published: November 2, 2023. doi:10.1001/jamanetworkopen.2023.41388

Open Access: This is an open access article distributed under the terms of the CC-BY License. © 2023 Thurston RC et al. JAMA Network Open.

Corresponding Author: Rebecca C. Thurston, PhD, Department of Psychiatry, University of Pittsburgh, 3811 O’Hara St, Pittsburgh, PA 15213 ([email protected]).

Author Contributions: Dr Thurston had full access to all of the data in the study and takes responsibility for the integrity of the data and the accuracy of the data analysis.

Concept and design: Thurston, Aizenstein, Koenen, Maki.

Acquisition, analysis, or interpretation of data: All authors.

Drafting of the manuscript: Thurston, Jakubowski.

Critical review of the manuscript for important intellectual content: All authors.

Statistical analysis: Chang.

Obtained funding: Thurston, Aizenstein, Koenen, Maki.

Administrative, technical, or material support: Thurston, Jakubowski, Wu, Aizenstein, Maki.

Supervision: Thurston, Aizenstein.

Conflict of Interest Disclosures: Dr Thurston reported receiving personal fees from Astellas Pharma, Bayer, Hello Therapeutics, Vira Health, and Happify Health outside the submitted work. Dr Maki reported receiving personal fees from Astellas, Bayer, Pfizer, and Mithra and having equity in Midi-Health, Estrigenix, and Alloy outside the submitted work. No other disclosures were reported.

Funding/Support: This research was supported by the National Institutes of Health (NIH), National Institute on Aging (grant No. RF1AG053504 and R01AG053504; Drs Thurston and Maki) and the NIH Heart Lung and Blood Institute (grant No. R01HL105647 and K24HL123565; Dr Thurston). This work was also supported by the University of Pittsburgh Clinical and Translational Science Institute (NIH grant No. UL1TR000005) and the University of Pittsburgh Small Molecule Biomarker Core (NIH grant No. S10RR023461).

Role of the Funder/Sponsor: The funders had no role in the design and conduct of the study; collection, management, analysis, and interpretation of the data; preparation, review, or approval of the manuscript; and decision to submit the manuscript for publication.

Data Sharing Statement: See Supplement 2.

References

1.

Virani
 SS, Alonso
 A, Aparicio
 HJ,
 et al; American Heart Association Council on Epidemiology and Prevention Statistics Committee and Stroke Statistics Subcommittee.  Heart disease and stroke statistics-2021 update: a report from the American Heart Association.   Circulation. 2021;143(8):e254-e743. doi:10.1161/CIR.0000000000000950 PubMedGoogle ScholarCrossref
2.

Heron
 M.  Deaths: leading causes for 2019.   Natl Vital Stat Rep. 2021;70(9):1-114.PubMedGoogle Scholar
3.

Rajan
 KB, Weuve
 J, Barnes
 LL, McAninch
 EA, Wilson
 RS, Evans
 DA.  Population estimate of people with clinical Alzheimer’s disease and mild cognitive impairment in the United States (2020-2060).   Alzheimers Dement. 2021;17(12):1966-1975. doi:10.1002/alz.12362 PubMedGoogle ScholarCrossref
4.

Resnick
 HS, Kilpatrick
 DG, Dansky
 BS, Saunders
 BE, Best
 CL.  Prevalence of civilian trauma and posttraumatic stress disorder in a representative national sample of women.   J Consult Clin Psychol. 1993;61(6):984-991. doi:10.1037/0022-006X.61.6.984 PubMedGoogle ScholarCrossref
6.

Jacquet-Smailovic
 M, Brennsthul
 MJ, Denis
 I, Kirche
 A, Tarquinio
 C, Tarquinio
 C.  Relationship between post-traumatic stress disorder and subsequent myocardial infarction: a systematic review and meta-analysis.   J Affect Disord. 2022;297:525-535. doi:10.1016/j.jad.2021.10.056 PubMedGoogle ScholarCrossref
8.

Flatt
 JD, Gilsanz
 P, Quesenberry
 CP
 Jr, Albers
 KB, Whitmer
 RA.  Post-traumatic stress disorder and risk of dementia among members of a health care delivery system.   Alzheimers Dement. 2018;14(1):28-34. doi:10.1016/j.jalz.2017.04.014 PubMedGoogle ScholarCrossref
9.

Lawn
 RB, Jha
 SC, Liu
 J,
 et al.  The association of posttraumatic stress disorder, depression, and head injury with mid-life cognitive function in civilian women.   Depress Anxiety. 2022;39(3):220-232. doi:10.1002/da.23233 PubMedGoogle ScholarCrossref
11.

Sumner
 JA, Hagan
 K, Grodstein
 F, Roberts
 AL, Harel
 B, Koenen
 KC.  Posttraumatic stress disorder symptoms and cognitive function in a large cohort of middle-aged women.   Depress Anxiety. 2017;34(4):356-366. doi:10.1002/da.22600 PubMedGoogle ScholarCrossref
12.

Anand
 SS, Islam
 S, Rosengren
 A,
 et al; INTERHEART Investigators.  Risk factors for myocardial infarction in women and men: insights from the INTERHEART study.   Eur Heart J. 2008;29(7):932-940. doi:10.1093/eurheartj/ehn018 PubMedGoogle ScholarCrossref
13.

Reiman
 EM, Quiroz
 YT, Fleisher
 AS,
 et al.  Brain imaging and fluid biomarker analysis in young adults at genetic risk for autosomal dominant Alzheimer’s disease in the presenilin 1 E280A kindred: a case-control study.   Lancet Neurol. 2012;11(12):1048-1056. doi:10.1016/S1474-4422(12)70228-4 PubMedGoogle ScholarCrossref
14.

El Khoudary
 SR, Wildman
 RP, Matthews
 K, Thurston
 RC, Bromberger
 JT, Sutton-Tyrrell
 K.  Progression rates of carotid intima-media thickness and adventitial diameter during the menopausal transition.   Menopause. 2013;20(1):8-14. doi:10.1097/gme.0b013e3182611787 PubMedGoogle ScholarCrossref
18.

Farrer
 LA, Cupples
 LA, Haines
 JL,
 et al; APOE and Alzheimer Disease Meta Analysis Consortium.  Effects of age, sex, and ethnicity on the association between apolipoprotein E genotype and Alzheimer disease: a meta-analysis.   JAMA. 1997;278(16):1349-1356. doi:10.1001/jama.1997.03550160069041 PubMedGoogle ScholarCrossref
20.

Stein
 JH, Korcarz
 CE, Hurst
 RT,
 et al; American Society of Echocardiography Carotid Intima-Media Thickness Task Force; Endorsed by the Society for Vascular Medicine.  Use of carotid ultrasound to identify subclinical vascular disease and evaluate cardiovascular disease risk: a consensus statement from the American Society of Echocardiography Carotid Intima-Media Thickness Task Force.   J Am Soc Echocardiogr. 2008;21(2):93-111. doi:10.1016/j.echo.2007.11.011 PubMedGoogle ScholarCrossref
21.

McClelland
 RL, Chung
 H, Detrano
 R, Post
 W, Kronmal
 RA.  Distribution of coronary artery calcium by race, gender, and age: results from the Multi-Ethnic Study of Atherosclerosis (MESA).   Circulation. 2006;113(1):30-37. doi:10.1161/CIRCULATIONAHA.105.580696 PubMedGoogle ScholarCrossref
22.

Debette
 S, Markus
 HS.  The clinical importance of white matter hyperintensities on brain magnetic resonance imaging: systematic review and meta-analysis.   BMJ. 2010;341:c3666. doi:10.1136/bmj.c3666 PubMedGoogle ScholarCrossref
24.

Thurston
 RC, El Khoudary
 SR, Tepper
 PG,
 et al; Appendix.  Trajectories of vasomotor symptoms and carotid intima media thickness in the Study of Women’s Health Across the Nation.   Stroke. 2016;47(1):12-17. doi:10.1161/STROKEAHA.115.010600 PubMedGoogle ScholarCrossref
26.

Lang
 AJ, Laffaye
 C, Satz
 LE, Dresselhaus
 TR, Stein
 MB.  Sensitivity and specificity of the PTSD checklist in detecting PTSD in female veterans in primary care.   J Trauma Stress. 2003;16(3):257-264. doi:10.1023/A:1023796007788 PubMedGoogle ScholarCrossref
30.

Wechsler
 D.  Wechsler Adult Intelligence Scale: Administration and Scoring Manual. 3rd ed. Harcourt Brace & Co; 1997.

31.

Smith
 A.  Symbol Digit Modalities Test. Western Psychological Services; 1973.

32.

French
 JW, Ekstrom
 RB, Price
 LA.  Manual for Kit of Reference Tests for Cognitive Factors. Educational Testing Service; 1963.

33.

Delis
 D, Kramer
 J, Kaplan
 E, Ober
 B.  California Verbal Learning Test: Adult Version Manual. 2nd ed. Harcourt-Brace; 2000.

35.

Kertesz
 A.  Western Aphasia Battery. The Psychological Corporation; 1982.

39.

Friedewald
 WT, Levy
 RI, Fredrickson
 DS.  Estimation of the concentration of low-density lipoprotein cholesterol in plasma, without use of the preparative ultracentrifuge.   Clin Chem. 1972;18(6):499-502. doi:10.1093/clinchem/18.6.499 PubMedGoogle ScholarCrossref
42.

Walczewska
 J, Rutkowski
 K, Wizner
 B, Cwynar
 M, Grodzicki
 T.  Stiffness of large arteries and cardiovascular risk in patients with post-traumatic stress disorder.   Eur Heart J. 2011;32(6):730-736. doi:10.1093/eurheartj/ehq354 PubMedGoogle ScholarCrossref
43.

Spitzer
 C, Klinger-König
 J, Frenzel
 S,
 et al.  Association of traumatic stress and posttraumatic stress disorder with carotid atherosclerosis: findings from the general population.   Eur J Psychotraumatol. 2020;11(1):1815280. doi:10.1080/20008198.2020.1815280 PubMedGoogle ScholarCrossref
44.

Lippa
 SM, Kenney
 K, Riedy
 G, Ollinger
 J.  White matter hyperintensities are not related to symptomatology or cognitive functioning in service members with a remote history of traumatic brain injury.   Neurotrauma Rep. 2021;2(1):245-254. doi:10.1089/neur.2021.0002 PubMedGoogle ScholarCrossref
45.

Scott
 JC, Matt
 GE, Wrocklage
 KM,
 et al.  A quantitative meta-analysis of neurocognitive functioning in posttraumatic stress disorder.   Psychol Bull. 2015;141(1):105-140. doi:10.1037/a0038039 PubMedGoogle ScholarCrossref
46.

Lyons
 MJ, Genderson
 M, Grant
 MD,
 et al.  Gene-environment interaction of ApoE genotype and combat exposure on PTSD.   Am J Med Genet B Neuropsychiatr Genet. 2013;162B(7):762-769. doi:10.1002/ajmg.b.32154 PubMedGoogle ScholarCrossref
47.

Mota
 NP, Han
 S, Harpaz-Rotem
 I,
 et al.  Apolipoprotein E gene polymorphism, trauma burden, and posttraumatic stress symptoms in U.S. military veterans: results from the National Health and Resilience in Veterans Study.   Depress Anxiety. 2018;35(2):168-177. doi:10.1002/da.22698 PubMedGoogle ScholarCrossref
48.

Averill
 LA, Abdallah
 CG, Levey
 DF,
 et al.  Apolipoprotein E gene polymorphism, posttraumatic stress disorder, and cognitive function in older U.S. veterans: results from the National Health and Resilience in Veterans Study.   Depress Anxiety. 2019;36(9):834-845. doi:10.1002/da.22912 PubMedGoogle ScholarCrossref
49.

Lawrence
 KA, Rippey
 CS, Welikson
 B, Pietrzak
 RH, Adams
 TG
 Jr.  Interactive association of posttraumatic stress disorder, apolipoprotein ε4 genotype, and age on cognitive functioning.   Int J Geriatr Psychiatry. 2023;38(2):e5888. doi:10.1002/gps.5888 PubMedGoogle ScholarCrossref
51.

Bradley
 SM, Stanislawski
 MA, Bekelman
 DB,
 et al.  Invasive coronary procedure use and outcomes among veterans with posttraumatic stress disorder: insights from the Veterans Affairs Clinical Assessment, Reporting, and Tracking Program.   Am Heart J. 2014;168(3):381-390.e6. doi:10.1016/j.ahj.2014.05.015 PubMedGoogle ScholarCrossref
53.

LeardMann
 CA, McMaster
 HS, Warner
 S,
 et al; Millennium Cohort Study Team.  Comparison of posttraumatic stress disorder checklist instruments From Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition vs Fifth Edition in a large cohort of US military service members and veterans.   JAMA Netw Open. 2021;4(4):e218072. doi:10.1001/jamanetworkopen.2021.8072PubMedGoogle ScholarCrossref

Leave a Reply

Your email address will not be published. Required fields are marked *