Clinical, genetic, and structural basis of apparent mineralocorticoid excess due to 11β-hydroxysteroid dehydrogenase type 2 deficiency

Yau, Mabel; Haider, Shozeb; Khattab, Ahmed; Ling, Chen; Mathew, Mehr; Zaidi, Samir; Bloch, Madison; Patel, Monica; Ewert, Sinead; Abdullah, Wafa; Toygar, A.; Mudryi, Vitalii; Badi, Maryam Al; Alzubdi, Mouch; Wilson, Robert; Azkawi, Hanan Said Al; Özdemir, Hatice; Abu‐Amer, Wahid; Hertecant, Jozef; Razzaghy-Azar, Maryam; Funder, John W.; Senani, Aisha Al; Sun, Li; Kim, Semin; Yuen, Tony; Zaidi, Mone; New, Maria I.

doi:10.1073/pnas.1716621115

Cited by 54 publications

(44 citation statements)

References 51 publications

(70 reference statements)

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“…Это редкое аутосомнорецессивное заболевание обычно протекает в форме тяжелой низкорениновой гипертонии и при отсутствии адекватного лечения приводит к фатальному исходу, хотя в некоторых случаях болезнь протекает в более мягкой форме. К настоящему времени обнаружено около 40 мутаций гена HSD11B2, которые могут приводить к формированию заболевания (Yau et al, 2017). Пациенты с выраженной симптоматикой имеют малый вес при рождении, артериальную гипертонию, полиурию и полидипсию, низкий уровень как ренина, так и альдостерона.…”

Section: наследственная низкорениновая гипертония без увеличения секрunclassified

Genetics and pathophysiology of low-renin arterial hypertension

Markel

2019

Vestn. VOGiS

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The review is devoted to the consideration of genetic determination and pathophysiology of one of the forms of hypertensive disease known as low-renin hypertension. At frst glance, the development of low-renin hypertension is “unnatural”, as renin, as a key enzyme of the renin-angiotensin system, which plays an important role in the development of hypertensive disease, is suppressed in low-renin hypertension. At the same time, the most important drugs actual in the treatment of hypertensive disease belong to the renin-angiotensin system blockers. This contradiction was resolved by a study of genetic and pathophysiological mechanisms of hypertension in some groups of patients with characteristic symptoms bringing these people together. Genetic studies of some recent decades using both family analysis and modern molecular genetic technologies have revealed the main mechanisms underlying low-renin hypertension, which can be classifed as certain syndromes with well-defned genetic and clinical features. These syndromes include cases of sporadically occurring somatic mutations in the cells of the adrenal cortex, which begin to produce aldosterone in increased amounts. Also, several oligogenic forms of low-renin hypertension were studied, some of which are associated with the hyperproduction of aldosterone, but in the others the development of low-renin hypertension was associated with mutations of genes involved in regulation of the functioning of the kidney ion channels. The discovery of some types of arterial hypertension with known mechanisms of their development is of paramount importance for medicine, as it allows for targeted efective therapy and in some cases for achieving a complete cure. However, the main contingent of patients with low-renin hypertension belongs to cases with unexplained etiology, as their development is associated with polygenic systems and with a signifcant inﬂuence of numerous environmental factors. The study of genetic and physiological mechanisms of various forms of low-renin arterial hypertension provides a good example of how penetration into the intimate mechanisms of the blood pressure regulation in each personal case makes it possible to identify some specifc syndromes and establish its fnal causes. It seems that progress in understanding the causes and mechanisms of essential hypertension lies along this way.

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Section: наследственная низкорениновая гипертония без увеличения секрunclassified

Genetics and pathophysiology of low-renin arterial hypertension

Markel

2019

Vestn. VOGiS

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“…Following the description of the first disease‐causing substitution, around 40 additional germline mutations have been reported, mainly in families where consanguineous marriages, endogamy or a founder effected had occurred . The recent development of a computational model of HSD11B2 protein provided a structural explanation for the genotype‐phenotype correlation and the clinical severity of AME syndrome, resulting from the reported mutations . In addition, the same model can be used to predict disease severity for novel described missense mutations in HSD11B2 …”

Section: Apparent Mineralocorticoid Excess Syndromementioning

confidence: 99%

“…The recent development of a computational model of HSD11B2 protein provided a structural explanation for the genotype‐phenotype correlation and the clinical severity of AME syndrome, resulting from the reported mutations . In addition, the same model can be used to predict disease severity for novel described missense mutations in HSD11B2 …”

Section: Apparent Mineralocorticoid Excess Syndromementioning

confidence: 99%

“…73 The recent development of a computational model of HSD11B2 protein provided a structural explanation for the genotype-phenotype correlation and the clinical severity of AME syndrome, resulting from the reported mutations. 78 In addition, the same model can be used to predict disease severity for novel described missense mutations in HSD11B2. 78 Biochemically, a markedly elevated urinary tetrahydrocortisol (THF, A-ring-reduced cortisol metabolite) + alloTHF to tetrahydrocortisone (THE, cortisol metabolite) [(THF+alloTHF)/THE] is the hallmark of the classical AME, 73,79 while patients with a mild form can display only a slightly increased ratio.…”

Section: Apparent Miner Alocorticoid E Xce Ss Syndromementioning

confidence: 99%

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Diagnostic approach to low‐renin hypertension

Monticone

Losano

Tetti

et al. 2018

Clinical Endocrinology

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Renin-angiotensin-aldosterone system (RAAS) plays a crucial role in maintaining water and electrolytes homoeostasis, and its deregulation contributes to the development of arterial hypertension. Since the historical description of the "classical" RAAS, a dramatic increase in our understanding of the molecular mechanisms underlying the development of both essential and secondary hypertension has occurred. Approximatively 25% of the patients affected by arterial hypertension display low-renin levels, a definition that is largely arbitrary and depends on the investigated population and the specific characteristics of the assay. Most often, low-renin levels are expression of a physiological response to sodium-volume overload, but also a significant number of secondary hereditary or acquired conditions falls within this category. In a context of suppressed renin status, the concomitant examination of plasma aldosterone levels (which can be inappropriately elevated, within the normal range or suppressed) and plasma potassium are essential to formulate a differential diagnosis. To distinguish between the different forms of low-renin hypertension is of fundamental importance to address the patient to the proper clinical management, as each subtype requires a specific and targeted therapy. The present review will discuss the differential diagnosis of the most common medical conditions manifesting with a clinical phenotype of low-renin hypertension, enlightening the novelties in genetics of the familial forms.

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“…11β-HSD2 inactivation results in physiological cortisol levels fully activating MR-driven kidney responses leading to aldosterone-independent MR activation. Indeed, inactivating mutations cause autosomal recessive AME, which disappears following kidney transplantation [ 12 ]. An elevation in the urinary tetrahydrocortisol (THF) plus allo-THF to tetrahydrocortisone (THE) [(THF + allo-THF)/THE] ratio is pathognomonic of homozygous inactivation, but it was reported to be less sensitive than a high serum cortisol/cortisone ratio to detect heterozygous subjects with milder enzyme deficiency [ 13 ].…”

Section: What Is 11β-hsd2?mentioning

confidence: 99%

Unravelling drug-induced hypertension: molecular mechanisms of aldosterone-independent mineralocorticoid receptor activation by posaconazole

Sanchez-Niño

Ortíz

2018

Clinical Kidney Journal

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Drug-induced hypertension offers the opportunity to further understand pathways involved in the regulation of blood pressure. Posaconazole is an antifungal agent known to induce hypertension and hypokalaemia. In recent months, a flurry of reports has unravelled the metabolic processes involved. In this issue of CKJ, Barton K, Davis TK, Marshall B et al. Posaconazole-induced hypertension and hypokalemia due to inhibition of the 11β-hydroxylase enzyme. Clin Kidney J 2018; 11: 691–693 present convincing evidence of 11β-hydroxylase inhibition resulting in a biochemical syndrome resembling genetic congenital adrenal hyperplasia and characterized by high 11-deoxycorticosterone and 11-deoxycortisol levels as well as androgen levels. This adds to prior evidence supporting inhibition of 11β-hydroxysteroid dehydrogenase 2, the enzyme that inactivates cortisol in aldosterone-sensitive tissues such as the kidneys, yielding a syndrome resembling genetic apparent mineralocorticoid excess or licorice toxicity, characterized by a high cortisol/cortisone ratio.

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Clinical, genetic, and structural basis of apparent mineralocorticoid excess due to 11β-hydroxysteroid dehydrogenase type 2 deficiency

Cited by 54 publications

References 51 publications

Genetics and pathophysiology of low-renin arterial hypertension

Genetics and pathophysiology of low-renin arterial hypertension

Diagnostic approach to low‐renin hypertension

Unravelling drug-induced hypertension: molecular mechanisms of aldosterone-independent mineralocorticoid receptor activation by posaconazole

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