Project background: This is a competing renewal R01 applicaton that proposes to study the cellular and genetic origins of the most common adrenal disease, primary aldosteronism (PA). The prevalence of PA is 6- 8% amongst all hypertensive patients suggesting that 1 in 40 American adults has PA. PA is hallmarked by renin-independent adrenal aldosterone production that results in excessive mineralocorticoid receptor (MR) activation. The two major subtypes of PA are unilateral aldosterone-producing adenoma (APA) and bilateral idiopathic hyperaldosteronism (IHA). While PA resulting from APA has a surgical cure, IHA requires life-long medical therapy using MR antagonists. There are no current therapeutic approaches that inhibit the disease- causing inappropriate aldosterone production in IHA patients. During the initial funding period of this grant, we made significant progress in defining genetic causes of PA. This includes the first in field use of a small cohort of IHA formalin-fixed paraffin-embedded (FFPE) adrenal tissues that showed a buildup of activating somatic mutations in CACNA1D (L-type calcium voltage-gated channel alpha 1D subunit). IHA CACNA1D mutations were found in aldosterone-producing cell clusters (APCC), a clonal adrenal dysplastic cellular entity that we initially described in the zona glomerulosa (ZG) of normal adrenals. These findings form the foundation for this competitive renewal application.
Specific Aims. Aim 1 will define the aldosterone-driving somatic mutations that initiate dysregulation of aldosterone production in a large cohort of normal adrenals (? 400).
Aim 2 will define the role of APCC and somatic gene mutations in bilateral adrenal IHA autonomous aldosterone production.
Aim 3 will evaluate the potential for calcium channel blockers (CCBs) to specifically target and reduce autonomous aldosterone secretion in patients with IHA. Overall significance and clinical impact. Despite the high prevalence of PA, its clear impact on cardiovascular disease, and intriguing new genetic findings related to its cause, we know very little about the origin and progression of PA and particularly IHA. Because IHA results from bilateral adrenal disease, there is no surgical cure. Current strategies, although effective, do not target dysregulation of aldosterone release but instead target the MR, which can cause unfavorable off target side effects. The proposed research would significantly improve our understanding of the molecular mechanisms causing bilateral adrenal IHA and has the added potential of providing foundational research for the development of novel therapeutics that could directly inhibit IHA adrenal renin-independent aldosterone production.

Public Health Relevance

Inappropriate production of aldosterone, the most common adrenal disease, causes hypertension, cardiovascular damage, and enchanced potential for metabolic syndrome. Recently, using a small cohort of adrenals from patients with primary aldosteronism due to bilateral idiopathic hyperaldosteronism (IHA), we identified a set of somatic mutations that causes autonomous aldosterone production. These findings form the foundation for this competitive renewal application that will test three hypotheses: i) due to the common nature of this disease, normal adrenals can be used to define the cellular origins and pathogenesis of primary aldosteronism resulting from somatic gene mutations (Aim 1), ii) IHA is caused by an expansion and accumulation of aldosterone-producing cell clusters that have somatic gene mutations in calcium channels (Aim 2), iii) the activating calcium channel mutations found in IHA adrenals provide a therapeutic target to inhibit the autonomous aldosterone production in IHA (Aim 3).

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK106618-06
Application #
10116368
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Malozowski, Saul N
Project Start
2016-03-01
Project End
2025-02-28
Budget Start
2021-03-01
Budget End
2022-02-28
Support Year
6
Fiscal Year
2021
Total Cost
Indirect Cost
Name
University of Michigan Ann Arbor
Department
Physiology
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109
Omata, Kei; Satoh, Fumitoshi; Morimoto, Ryo et al. (2018) Cellular and Genetic Causes of Idiopathic Hyperaldosteronism. Hypertension 72:874-880
Nanba, Kazutaka; Vaidya, Anand; Rainey, William E (2018) Aging and Adrenal Aldosterone Production. Hypertension 71:218-223
Nanba, Kazutaka; Omata, Kei; Else, Tobias et al. (2018) Targeted Molecular Characterization of Aldosterone-Producing Adenomas in White Americans. J Clin Endocrinol Metab 103:3869-3876
Sun, Na; Wu, Yin; Nanba, Kazutaka et al. (2018) High-Resolution Tissue Mass Spectrometry Imaging Reveals a Refined Functional Anatomy of the Human Adult Adrenal Gland. Endocrinology 159:1511-1524
Omata, Kei; Anand, Sharath K; Hovelson, Daniel H et al. (2017) Aldosterone-Producing Cell Clusters Frequently Harbor Somatic Mutations and Accumulate With Age in Normal Adrenals. J Endocr Soc 1:787-799
Omata, Kei; Tomlins, Scott A; Rainey, William E (2017) Aldosterone-Producing Cell Clusters in Normal and Pathological States. Horm Metab Res 49:951-956
Omata, Kei; Yamazaki, Yuto; Nakamura, Yasuhiro et al. (2017) Genetic and Histopathologic Intertumor Heterogeneity in Primary Aldosteronism. J Clin Endocrinol Metab 102:1792-1796
Yamazaki, Yuto; Nakamura, Yasuhiro; Omata, Kei et al. (2017) Histopathological Classification of Cross-Sectional Image-Negative Hyperaldosteronism. J Clin Endocrinol Metab 102:1182-1192
Nanba, Kazutaka; Vaidya, Anand; Williams, Gordon H et al. (2017) Age-Related Autonomous Aldosteronism. Circulation 136:347-355
Nanba, Kazutaka; Chen, Andrew X; Omata, Kei et al. (2016) Molecular Heterogeneity in Aldosterone-Producing Adenomas. J Clin Endocrinol Metab 101:999-1007

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