Hypertension (HTN) contributes disproportionately to the global burden of disease. In our prior application, we have provided evidence for an important link between particulate matter <2.5 mm (PM2.5) exposure and development of HTN. In this competitive renewal application, we propose to further investigate these links in the context of our findings that inflammation mediated sympathetic nervous system (SNS) activation in circumventricular organs (CVO) in the brain represent an integrative mechanism for PM2.5 induced HTN. Our hypothesis is consistent with an evolving shift in our understanding of the SNS as an arbitrator of acute tonal changes in HTN to a facilitator of chronic functional and structural changes via immune mechanisms. We propose to test this hypothesis in both animal models and humans as part of our established inter-disciplinary collaborative group.
In aim 1, we will investigate the time course, loci and impact of central nervous system (CNS) inflammation on BP with PM2.5 exposure conducted in a versatile aerosol concentration enrichment system (VACES) using C57/Bl6 and NFkB reporter mice. We will directly assess the impact of PM2.5 in exaggerating BP using a model of central SNS activation and also assess the impact of activating inflammation proximally on SNS activation on BP response to FA/PM2.5. Dose response studies and analysis of PM2.5 components responsible for HTN, will be performed in pre-disposed models.
In Aim 2, the role of central TLR activation in the CVO organs will be tested by deleting TNF receptor-associated factor (TRAF6), selectively in the CVO using UbcCre-TRAF6flox/flox(TRAF6pCNS) mice using Tamoxifen injected intra-cerebroventricularly (ICV), followed by exposure to FA/PM2.5. TRAF6 is a unique member of the TRAF family that functions at nodal points where signals induced via multiple TLRs converge. We will additionally distinguish between neuronal and glial cell specific role of TRAF6 in CNS inflammation in response to PM2.5.
In Aim 3, we will test the involvement of central SNS as a relevant pathway in humans, exposed to sub-acute time periods to ambient PM2.5, as part of a blinded randomized cross-over intervention. Our hypothesis is that Guanfacine an approved a2A agonist will obviate the association of ambient PM2.5 with 24-hour ambulatory systolic BP and SNS activity measured by HRV measures. Our experiments are highly relevant to continuing risk posed by air- pollution to people living in urbanized environments.

Public Health Relevance

Particulate matter air-pollution is a major cause of global cardiovascular morbidity and mortality. In our previous submission we have demonstrated that a major component of air-pollution (particulate matter <2.5 ? micron in size (PM2.5) contributes to increases in blood pressure in both animals and humans. In this continuation grant we will investigate broad integrative mechanisms by which PM2.5 may facilitate development of hypertension and thereby contribute to cardiovascular events. We propose to test this association in novel animal models of susceptibility that mirror the human condition. We will also test the effect of a drug called Guanfacine in susceptible humans to see if this intervention can prevent increases in blood pressure associated with elevated levels of personal PM2.5 exposure.

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
5R01ES015146-10
Application #
9492563
Study Section
Clinical and Integrative Cardiovascular Sciences Study Section (CICS)
Program Officer
Schug, Thaddeus
Project Start
2007-04-01
Project End
2019-05-31
Budget Start
2018-06-01
Budget End
2019-05-31
Support Year
10
Fiscal Year
2018
Total Cost
Indirect Cost
Name
Case Western Reserve University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106
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Ying, Zhekang; Chen, Minjie; Xie, Xiaoyun et al. (2016) Lipoicmethylenedioxyphenol Reduces Experimental Atherosclerosis through Activation of Nrf2 Signaling. PLoS One 11:e0148305

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