Department of Clinical, Internal, Anaesthesiologic and Cardiovascular Sciences, 'Sapienza', Rome University, Rome, Italy.
Center for Molecular Oncology and Division of Endocrinology & Metabolism, University of Connecticut School of Medicine, Farmington, CT, USA.
J Bone Miner Res. 2022 Nov;37(11):2315-2329. doi: 10.1002/jbmr.4665. Epub 2022 Oct 17.
In this narrative review, we present data gathered over four decades (1980-2020) on the epidemiology, pathophysiology and genetics of primary hyperparathyroidism (PHPT). PHPT is typically a disease of postmenopausal women, but its prevalence and incidence vary globally and depend on a number of factors, the most important being the availability to measure serum calcium and parathyroid hormone levels for screening. In the Western world, the change in presentation to asymptomatic PHPT is likely to occur, over time also, in Eastern regions. The selection of the population to be screened will, of course, affect the epidemiological data (ie, general practice as opposed to tertiary center). Parathyroid hormone has a pivotal role in regulating calcium homeostasis; small changes in extracellular Ca++ concentrations are detected by parathyroid cells, which express calcium-sensing receptors (CaSRs). Clonally dysregulated overgrowth of one or more parathyroid glands together with reduced expression of CaSRs is the most important pathophysiologic basis of PHPT. The spectrum of skeletal disease reflects different degrees of dysregulated bone remodeling. Intestinal calcium hyperabsorption together with increased bone resorption lead to increased filtered load of calcium that, in addition to other metabolic factors, predispose to the appearance of calcium-containing kidney stones. A genetic basis of PHPT can be identified in about 10% of all cases. These may occur as a part of multiple endocrine neoplasia syndromes (MEN1-MEN4), or the hyperparathyroidism jaw-tumor syndrome, or it may be caused by nonsyndromic isolated endocrinopathy, such as familial isolated PHPT and neonatal severe hyperparathyroidism. DNA testing may have value in: confirming the clinical diagnosis in a proband; eg, by distinguishing PHPT from familial hypocalciuric hypercalcemia (FHH). Mutation-specific carrier testing can be performed on a proband's relatives and identify where the proband is a mutation carrier, ruling out phenocopies that may confound the diagnosis; and potentially prevention via prenatal/preimplantation diagnosis. © 2022 The Authors. Journal of Bone and Mineral Research published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research (ASBMR).
在这篇叙述性综述中,我们呈现了四十年来(1980-2020 年)收集的关于原发性甲状旁腺功能亢进症(PHPT)的流行病学、病理生理学和遗传学数据。PHPT 通常是绝经后妇女的疾病,但它的患病率和发病率在全球范围内有所不同,这取决于许多因素,最重要的是是否有条件进行血清钙和甲状旁腺激素水平的筛查。在西方国家,无症状 PHPT 的表现也可能随着时间的推移在东方地区发生变化。筛查人群的选择当然会影响流行病学数据(即一般实践与三级中心相比)。甲状旁腺激素在调节钙稳态中起着关键作用;细胞外 Ca++浓度的微小变化被甲状旁腺细胞检测到,甲状旁腺细胞表达钙敏感受体(CaSRs)。一个或多个甲状旁腺的克隆性失调性过度生长以及 CaSRs 的表达减少是 PHPT 的最重要病理生理基础。骨骼疾病的谱反映了不同程度的失调性骨重塑。肠道钙吸收增加以及骨吸收增加导致钙过滤负荷增加,除了其他代谢因素外,还会导致含钙肾结石的出现。大约 10%的 PHPT 病例可以确定其遗传基础。这些可能作为多发性内分泌肿瘤综合征(MEN1-MEN4)的一部分发生,或者甲状旁腺功能亢进颌骨肿瘤综合征,或者可能由非综合征孤立性内分泌病引起,如家族性孤立性甲状旁腺功能亢进症和新生儿严重甲状旁腺功能亢进症。DNA 检测可能具有以下价值:在患者中确认临床诊断;例如,通过将 PHPT 与家族性低钙尿性高钙血症(FHH)区分开来。可以对患者的亲属进行突变特异性携带者检测,并确定患者是否为突变携带者,排除可能使诊断复杂化的表型;并可能通过产前/植入前诊断进行预防。© 2022 作者。《骨与矿物研究杂志》由 Wiley 期刊公司代表美国骨与矿物研究协会(ASBMR)出版。
