# BLR&D Research Career Scientist Award

> **NIH VA IK6** · OMAHA VA  MEDICAL CENTER · 2021 · —

## Abstract

My primary research interests address chronic inflammatory lung diseases and the
impact that environmental exposures play in the compromise of lung innate defense
against pathologic lung injury. Utilizing pre-clinical mouse models and state-of-the-art
molecular, biochemical, and cellular approaches, I collaborate closely with
pulmonologists who practice at the VA to conduct relevant pre-clinical research that can
be used to address current clinical concerns. Listed below is a summary of my VA-
funded research project:
Malondialdehyde-acetaldehyde adducts and lung injury. Alcohol abuse causing
increased susceptibility to pneumonia has been known for over 200 years. Hospitalized
individuals with alcohol use disorders (AUDs) have a 3-fold risk of mortality from
pneumonia. Alcohol modulates both the innate and adaptive immune systems of the
lung resulting in increased susceptibility and decreased resolution of infection. Because
the majority (>90%) individuals with AUDs smoke cigarettes, we have chosen to take
the public health relevant approach of studying the combination lung injury effects of
both cigarettes and alcohol. In our previous funding cycle, we identified that the lungs
represent a unique environment for the formation of stable malondialdehyde-
acetaldehyde protein adducts (MAA adducts), but only under conditions of combined
cigarette smoke and alcohol exposure. These MAA adducts cause airway epithelial cell
cilia slowing and impair the innate pathogen clearance from the lung. Our published and
preliminary data demonstrate that surfactant protein D (SPD) is a major lung protein that
gets adducted when lung aldehyde concentrations are elevated during combined smoke
and alcohol exposure. Using human samples derived from the NIAAA-supported
Colorado Pulmonary Alcohol Research Consortium, we have found that MAA adducts
are detected in the lung lavage macrophages and fluid only in individuals with AUDs
who also smoke. We have observed that the AUD smokers have decreased lung
mucosal sIgA and that MAA adduct treatment of airway epithelium blocks transcytotic
processing of sIgA mucosal secretion. Because of these important and novel
observations, we now propose to extend our research on the pathogenesis of the MAA
adduct to lung macrophages, mucosal sIgA, and SPD. Our overall hypothesis is that
MAA adducts uniquely form in the lungs of individuals who consume both alcohol and
smoke cigarettes, leading to alterations in innate lung defense. We will investigate this
hypothesis through 3 aims: Aim 1: MAA adducted lung SPD (MAA-SPD) binds to lung
macrophages via scavenger receptor A leading to alterations in macrophage function;
Aim 2: MAA-SPD prevents sIgA mucosal secretion in lung by altering epithelial cell
processing of dimerized IgA; and Aim 3: MAA adduction of SPD decreases its anti-
microbial action (Funded by the Department of Veterans Affairs Merit Award: VA I01
BX003635; 2016-2020).

## Key facts

- **NIH application ID:** 10265367
- **Project number:** 5IK6BX003781-05
- **Recipient organization:** OMAHA VA  MEDICAL CENTER
- **Principal Investigator:** Todd A Wyatt
- **Activity code:** IK6 (R01, R21, SBIR, etc.)
- **Funding institute:** VA
- **Fiscal year:** 2021
- **Award amount:** —
- **Award type:** 5
- **Project period:** 2017-04-01 → 2022-03-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10265367

## Citation

> US National Institutes of Health, RePORTER application 10265367, BLR&D Research Career Scientist Award (5IK6BX003781-05). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10265367. Licensed CC0.

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