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91 Agent Orange Exposure and Mild Cognitive Impairment in U.S. Vietnam Era Veterans

Published online by Cambridge University Press:  21 December 2023

Rosemary Toomey*
Affiliation:
Boston University Department of Psychological and Brain Sciences, Boston, MA, USA.
Carol E Franz
Affiliation:
University of California San Diego Department of Psychiatry, La Jolla, CA, USA. University of California San Diego Center for Behavior Genetics of Aging, La Jolla, CA, USA
Jeremy A Elman
Affiliation:
University of California San Diego Department of Psychiatry, La Jolla, CA, USA. University of California San Diego Center for Behavior Genetics of Aging, La Jolla, CA, USA
Ruth E McKenzie
Affiliation:
Boston University Department of Psychological and Brain Sciences, Boston, MA, USA.
William S Kremen
Affiliation:
University of California San Diego Department of Psychiatry, La Jolla, CA, USA. University of California San Diego Center for Behavior Genetics of Aging, La Jolla, CA, USA
Michael J Lyons
Affiliation:
Boston University Department of Psychological and Brain Sciences, Boston, MA, USA.
*
Correspondence: Rosemary Toomey, Ph.D. Boston University Department of Psychological and Brain Sciences toomey@bu.edu
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Abstract

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Objective:

US forces used Agent Orange (AO) during the Vietnam War and continued to store/test it at other locations after the war. AO is a powerful herbicide including dioxin, a highly toxic ingredient classified as a human carcinogen. The National Academies of Sciences, Engineering, and Medicine periodically review the literature on the health effects of AO exposure (AOE) and concluded in 2018 that there is sufficient evidence linking AO with a wide range of adverse health outcomes, including neurologic disorders (e.g., Parkinson’s disease). The VA has a list of medical disorders considered presumptive conditions related to AOE. More recently, AOE has been linked to a nearly double risk compared to those without AOE for receiving a dementia diagnosis. To our knowledge, no one has investigated the association of AOE to mild cognitive impairment (MCI), a condition thought to precede dementia.

Participants and Methods:

We examined men in three waves of the Vietnam Era Twin Study of Aging (VETSA). In wave 3, participants self-reported yes/no to the question of whether they ever had prolonged or serious AOE. MCI was diagnosed by the Jak-Bondi approach. Impairment was defined as 2+ tests within a cognitive domain that were more than 1.5 standard deviations below normative means after adjusting for premorbid cognitive ability. In mixed effects models, we tested the effect of AOE on MCI status. Models were adjusted for age, ethnicity, and non-independence within twin pairs.

Results:

In wave 3, 12.6% (230) of 1167 participants reported AOE. Those with AOE data had mean ages of 51.1 (wave 1), 56.0 (wave 2), and 61.4 (wave 3). Those with data on both AOE and MCI numbered 861 (wave 1), 900 (wave 2), 1121 (wave 3), and 766 had AOE and MCI at all waves. AOE was significantly related to wave 2 MCI (p < .001), but not to waves 1 and 3 MCI. AOE was significantly associated with the number of time points at which someone met criteria for MCI (p = .011). Analyses were conducted on six cognitive domains used to diagnose MCI, using available participants per wave. At all 3 waves, AOE was significantly associated with lower scores in processing speed (p = .003, p = .004, p = .005, respectively), working memory (p < .001, p = .002, p = .008) and nearly significant at all waves for executive dysfunction (p < .001, p < .001, p = .050). There were two other significant associations [wave 2 memory (p = .038), wave 3 fluency (p = .024)]. The semantic fluency cognitive domain was unrelated to AOE in all waves.

Conclusions:

AOE was consistently associated with lower processing speed, working memory, and executive dysfunction in males ages 51-61. It was also associated with the number of time points at which one met criteria for MCI in that age range, and with MCI in the mid-fifties. Findings support the idea of a risk for greater cognitive decline in those exposed to AO earlier in their lives, and with a risk for developing MCI.

Type
Poster Session 04: Aging | MCI
Copyright
Copyright © INS. Published by Cambridge University Press, 2023