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Literature DB >> 28447626

Familial hyperaldosteronism type III.

S Monticone¹, M Tetti¹, J Burrello¹, F Buffolo¹, R De Giovanni², F Veglio¹, T A Williams^1,3, P Mulatero¹.

Abstract

Primary aldosteronism is the most common form of endocrine hypertension. This disorder comprises both sporadic and familial forms. Four familial forms of primary aldosteronism (FH-I to FH-IV) have been described. FH-III is caused by germline mutations in KCNJ5, encoding the potassium channel Kir3.4 (also called GIRK4). These mutations alter the selectivity filter of the channel and lead to abnormal ion currents with loss of potassium selectivity, sodium influx and consequent increased intracellular calcium that causes excessive aldosterone biosynthesis. To date, eleven families have been reported, carrying six different mutations. Although the clinical features are variable, FH-III patients often display severe hyperaldosteronism with an early onset, associated with hypokalemia and diabetes insipidus-like symptoms. In most cases FH-III patients are resistant to pharmacological therapy and require bilateral adrenalectomy to control symptoms. In the present manuscript, we review the genetics and pathological basis of FH-III, the diagnostic work-up, clinical features and therapeutic management. Finally, we will describe a new case of FH-III of an Italian patient carrying a Gly151Arg mutation.

Entities: Chemical Disease Gene Species

Mesh：

Substances：

Year: 2017 PMID： 28447626 DOI： 10.1038/jhh.2017.34

Source DB: PubMed Journal: J Hum Hypertens ISSN： 0950-9240 Impact factor: 3.012

35 in total

1. Effect of KCNJ5 mutations on gene expression in aldosterone-producing adenomas and adrenocortical cells.

Authors: Silvia Monticone; Namita G Hattangady; Koshiro Nishimoto; Franco Mantero; Beatrice Rubin; Maria Verena Cicala; Raffaele Pezzani; Richard J Auchus; Hans K Ghayee; Hirotaka Shibata; Isao Kurihara; Tracy A Williams; Judith G Giri; Roni J Bollag; Michael A Edwards; Carlos M Isales; William E Rainey
Journal: J Clin Endocrinol Metab Date: 2012-05-24 Impact factor: 5.958

2. Hypertension with or without adrenal hyperplasia due to different inherited mutations in the potassium channel KCNJ5.

Authors: Ute I Scholl; Carol Nelson-Williams; Peng Yue; Roger Grekin; Robert J Wyatt; Michael J Dillon; Robert Couch; Lisa K Hammer; Frances L Harley; Anita Farhi; Wen-Hui Wang; Richard P Lifton
Journal: Proc Natl Acad Sci U S A Date: 2012-01-30 Impact factor: 11.205

3. Clinical and pathological diversity of primary aldosteronism, including a new familial variety.

Authors: R D Gordon; M Stowasser; T J Tunny; S A Klemm; W L Finn; A L Krek
Journal: Clin Exp Pharmacol Physiol Date: 1991-05 Impact factor: 2.557

Review 4. Study Heterogeneity and Estimation of Prevalence of Primary Aldosteronism: A Systematic Review and Meta-Regression Analysis.

Authors: Sabine C Käyser; Tanja Dekkers; Hans J Groenewoud; Gert Jan van der Wilt; J Carel Bakx; Mark C van der Wel; Ad R Hermus; Jacques W Lenders; Jaap Deinum
Journal: J Clin Endocrinol Metab Date: 2016-05-12 Impact factor: 5.958

5. Specific pattern of ionic channel gene expression associated with pacemaker activity in the mouse heart.

Authors: Céline Marionneau; Brigitte Couette; Jie Liu; Huiyu Li; Matteo E Mangoni; Joël Nargeot; Ming Lei; Denis Escande; Sophie Demolombe
Journal: J Physiol Date: 2004-10-21 Impact factor: 5.182

6. K+ channel mutations in adrenal aldosterone-producing adenomas and hereditary hypertension.

Authors: Murim Choi; Ute I Scholl; Peng Yue; Peyman Björklund; Bixiao Zhao; Carol Nelson-Williams; Weizhen Ji; Yoonsang Cho; Aniruddh Patel; Clara J Men; Elias Lolis; Max V Wisgerhof; David S Geller; Shrikant Mane; Per Hellman; Gunnar Westin; Göran Åkerström; Wenhui Wang; Tobias Carling; Richard P Lifton
Journal: Science Date: 2011-02-11 Impact factor: 47.728

Review 7. Role of KCNJ5 in familial and sporadic primary aldosteronism.

Authors: Paolo Mulatero; Silvia Monticone; William E Rainey; Franco Veglio; Tracy Ann Williams
Journal: Nat Rev Endocrinol Date: 2012-12-11 Impact factor: 43.330

8. A chimaeric 11 beta-hydroxylase/aldosterone synthase gene causes glucocorticoid-remediable aldosteronism and human hypertension.

Authors: R P Lifton; R G Dluhy; M Powers; G M Rich; S Cook; S Ulick; J M Lalouel
Journal: Nature Date: 1992-01-16 Impact factor: 49.962

Review 9. An Update on Familial Hyperaldosteronism.

Authors: H E Korah; U I Scholl
Journal: Horm Metab Res Date: 2015-10-07 Impact factor: 2.936

10. The potassium channel, Kir3.4 participates in angiotensin II-stimulated aldosterone production by a human adrenocortical cell line.

Authors: Kenji Oki; Maria W Plonczynski; Milay Luis Lam; Elise P Gomez-Sanchez; Celso E Gomez-Sanchez
Journal: Endocrinology Date: 2012-07-13 Impact factor: 4.736

7 in total

Review 1. Familial hyperaldosteronism type III a novel case and review of literature.

Authors: Natividad Pons Fernández; Francisca Moreno; Julia Morata; Ana Moriano; Sara León; Carmen De Mingo; Ángel Zuñiga; Fernando Calvo
Journal: Rev Endocr Metab Disord Date: 2019-03 Impact factor: 6.514

2. Primary Aldosteronism: KCNJ5 Mutations and Adrenocortical Cell Growth.

Authors: Yuhong Yang; Celso E Gomez-Sanchez; Diana Jaquin; Elke Tatjana Aristizabal Prada; Lucie S Meyer; Thomas Knösel; Holger Schneider; Felix Beuschlein; Martin Reincke; Tracy Ann Williams
Journal: Hypertension Date: 2019-08-26 Impact factor: 10.190

Familial hyperaldosteronism type III.

1. Effect of KCNJ5 mutations on gene expression in aldosterone-producing adenomas and adrenocortical cells.

2. Hypertension with or without adrenal hyperplasia due to different inherited mutations in the potassium channel KCNJ5.

3. Clinical and pathological diversity of primary aldosteronism, including a new familial variety.

Review 4. Study Heterogeneity and Estimation of Prevalence of Primary Aldosteronism: A Systematic Review and Meta-Regression Analysis.

5. Specific pattern of ionic channel gene expression associated with pacemaker activity in the mouse heart.

6. K+ channel mutations in adrenal aldosterone-producing adenomas and hereditary hypertension.

Review 7. Role of KCNJ5 in familial and sporadic primary aldosteronism.

8. A chimaeric 11 beta-hydroxylase/aldosterone synthase gene causes glucocorticoid-remediable aldosteronism and human hypertension.

Review 9. An Update on Familial Hyperaldosteronism.

10. The potassium channel, Kir3.4 participates in angiotensin II-stimulated aldosterone production by a human adrenocortical cell line.

Review 1. Familial hyperaldosteronism type III a novel case and review of literature.

2. Primary Aldosteronism: KCNJ5 Mutations and Adrenocortical Cell Growth.

Review 3. Pathophysiology of bilateral hyperaldosteronism.

4. Mosaicism for KCNJ5 Causing Early-Onset Primary Aldosteronism due to Bilateral Adrenocortical Hyperplasia.

Review 5. Who should be screened for primary aldosteronism? A comprehensive review of current evidence.

Review 6. Diseases caused by mutations in the Na⁺/K⁺ pump α1 gene ATP1A1.

Review 7. Comparative Genomics and Transcriptome Profiling in Primary Aldosteronism.

Review 4. Study Heterogeneity and Estimation of Prevalence of Primary Aldosteronism: A Systematic Review and Meta-Regression Analysis.

Review 7. Role of KCNJ5 in familial and sporadic primary aldosteronism.

Review 9. An Update on Familial Hyperaldosteronism.

Review 1. Familial hyperaldosteronism type III a novel case and review of literature.

Review 3. Pathophysiology of bilateral hyperaldosteronism.

Review 5. Who should be screened for primary aldosteronism? A comprehensive review of current evidence.

Review 6. Diseases caused by mutations in the Na+/K+ pump α1 gene ATP1A1.

Review 7. Comparative Genomics and Transcriptome Profiling in Primary Aldosteronism.

Review 6. Diseases caused by mutations in the Na⁺/K⁺ pump α1 gene ATP1A1.