Primary Aldosteronism: An Endocrine Society Clinical Practice Guideline.

Gail K Adler, Michael Stowasser, Ricardo R Correa, Nadia Khan, Gregory Kline, Michael J McGowan, Paolo Mulatero, M Hassan Murad, Rhian M Touyz, Anand Vaidya, Tracy A Williams, Jun Yang, William F Young, Maria-Christina Zennaro, Juan P Brito
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引用次数: 0

Abstract

Background: Primary aldosteronism (PA), a primary adrenal disorder leading to excessive aldosterone production by one or both adrenal glands, is a common cause of hypertension. It is associated with an increased risk of cardiovascular complications compared with primary hypertension. Despite effective methods for diagnosing and treating PA, it remains markedly underdiagnosed and undertreated.

Objective: To develop an updated guideline that provides a practical, clinical approach to identifying and managing PA to improve diagnosis rates and encourage targeted treatment.

Methods: The Guideline Development Panel (GDP), composed of a multidisciplinary panel of clinical experts and experts in systemic review methodology, used the Grading of Recommendations, Assessment, Development, and Evaluation (GRADE) approach to define 10 questions related to the diagnosis and treatment of PA. Systematic reviews were conducted for each question. The GDP used the GRADE Evidence to Decision (EtD) framework to consider contextual factors, such as stakeholder values and preferences, costs and required resources, cost-effectiveness, acceptability, feasibility, and the potential impact on health equity.

Results: We suggest that all individuals with hypertension be screened for PA by measuring aldosterone and renin and determining the aldosterone to renin ratio, and that subsequent clinical care be guided by the results. We suggest that individuals with PA receive PA-specific therapy, either medical or surgical. In individuals who screen positive for PA, we suggest (1) commencement of PA-specific medical therapy in individuals who do not desire or are not candidates for surgery and in situations where the probability of lateralizing PA (excess aldosterone produced by one adrenal) is low based on screening results; and (2) aldosterone suppression testing in situations when screening results indicate an intermediate probability for lateralizing PA and individualized decision making confirms a desire to pursue eligibility for surgical therapy. In those who test positive by aldosterone suppression testing, and in those in whom screening results show a high probability of lateralizing PA (obviating the need for aldosterone suppression testing), we suggest adrenal lateralization with computed tomography scanning and adrenal venous sampling prior to deciding the treatment approach (medical vs surgical). In all individuals with PA and an adrenal adenoma, we suggest performing a 1-mg overnight dexamethasone suppression test. We suggest the use of mineralocorticoid receptor antagonists (MRAs) over epithelial sodium-channel (ENaC) inhibitors in the medical treatment of PA. We suggest the use of spironolactone over other MRAs, given its lower cost and greater availability; however, all MRAs, when titrated to equivalent potencies, are anticipated to have similar efficacy in treating PA. Thus, MRAs with greater mineralocorticoid receptor specificity and fewer androgen/progesterone receptor-mediated side effects may be preferred in some situations. In individuals receiving MRA therapy, we suggest monitoring renin and, in those whose hypertension remains uncontrolled and renin is suppressed, titrating the MRA to increase renin.

Conclusion: These recommendations provide a practical framework for the diagnosis and treatment of PA. They are based on currently available literature and take into consideration outcomes that are important to key stakeholders. The goal is to increase identification of individuals with PA and, by initiating PA-specific medical or surgical therapy, improve blood pressure control and reduce PA-associated adverse cardiovascular events. The guidelines also highlight important knowledge gaps in PA diagnosis and management.

原发性醛固酮增多症:内分泌学会临床实践指南。
背景:原发性醛固酮增多症(PA)是一种原发性肾上腺疾病,导致一个或两个肾上腺产生过多的醛固酮,是高血压的常见原因。与原发性高血压相比,它与心血管并发症的风险增加有关。尽管有有效的诊断和治疗方法,但它仍然明显未被诊断和治疗。目的:制定一个更新的指南,提供一个实用的临床方法来识别和管理PA,以提高诊断率和鼓励有针对性的治疗。方法:指南制定小组(GDP)由临床专家和系统评价方法学专家组成的多学科小组,采用推荐、评估、发展和评价分级(GRADE)方法定义了与PA诊断和治疗相关的10个问题。对每个问题进行系统评价。GDP使用GRADE决策证据(EtD)框架来考虑相关因素,如利益相关者的价值观和偏好、成本和所需资源、成本效益、可接受性、可行性以及对卫生公平的潜在影响。结果:我们建议所有高血压患者通过测量醛固酮和肾素并确定醛固酮与肾素的比值来筛查PA,并以结果为指导进行后续临床护理。我们建议PA患者接受PA特异性治疗,无论是药物治疗还是手术治疗。对于PA筛查呈阳性的个体,我们建议(1)对于不希望或不适合手术的个体,以及根据筛查结果,侧化PA(由一个肾上腺产生的过量醛固酮)的可能性较低的情况,开始进行PA特异性药物治疗;(2)醛固酮抑制试验,当筛选结果表明有偏侧性前列腺炎的中等概率,并且个性化决策确认了追求手术治疗资格的愿望时。对于醛固酮抑制试验呈阳性的患者,以及筛查结果显示侧化肾上腺皮质激素可能性较高的患者(无需醛固酮抑制试验),我们建议在决定治疗方法(药物或手术)之前,通过计算机断层扫描和肾上腺静脉取样进行肾上腺侧化。在所有PA和肾上腺腺瘤患者中,我们建议进行1毫克地塞米松抑制试验。我们建议在PA的医学治疗中使用矿皮质激素受体拮抗剂(MRAs)而不是上皮钠通道(ENaC)抑制剂。我们建议使用螺内酯而不是其他mra,因为它的成本更低,可获得性更高;然而,所有的mra,当滴定到相同的效力时,预计在治疗PA方面具有相似的疗效。因此,在某些情况下,具有更大的矿皮质激素受体特异性和较少雄激素/孕激素受体介导的副作用的mra可能是首选。在接受MRA治疗的个体中,我们建议监测肾素,在高血压不受控制且肾素被抑制的患者中,滴定MRA以增加肾素。结论:这些建议为前列腺癌的诊断和治疗提供了一个实用的框架。它们以当前可用的文献为基础,并考虑到对关键利益相关者重要的结果。目的是增加对PA患者的识别,并通过启动PA特异性的药物或手术治疗,改善血压控制,减少PA相关的不良心血管事件。该指南还强调了PA诊断和管理方面的重要知识差距。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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