遗传性白细胞介素-12缺乏症:来自六个家族的13例患者的IL12B基因型和临床表型
Inherited interleukin-12 deficiency: IL12B genotype and clinical phenotype of 13 patients from six kindreds.
作者信息
Picard Capucine, Fieschi Claire, Altare Frédéric, Al-Jumaah Suliman, Al-Hajjar Sami, Feinberg Jacqueline, Dupuis Stéphanie, Soudais Claire, Al-Mohsen Ibrahim Zaid, Génin Emmanuelle, Lammas David, Kumararatne Dinakantha S, Leclerc Tony, Rafii Arash, Frayha Husn, Murugasu Belinda, Wah Lee Bee, Sinniah Raja, Loubser Michael, Okamoto Emi, Al-Ghonaium Abdulaziz, Tufenkeji Haysam, Abel Laurent, Casanova Jean-Laurent
机构信息
Laboratoire de Génétique Humaine des Maladies Infectieuses, Université René Descartes INSERM U550, Faculté de Médecine Necker, Paris, France.
出版信息
Am J Hum Genet. 2002 Feb;70(2):336-48. doi: 10.1086/338625. Epub 2001 Dec 17.
Interleukin-12 (IL12) is a cytokine that is secreted by activated phagocytes and dendritic cells and that induces interferon-gamma production by natural-killer and T lymphocytes. It consists of two subunits, p35 and p40, which are encoded by IL12A and IL12B, respectively. The first reported patient with a genetic cytokine disorder was a Pakistani child, who was homozygous for a large loss-of-function deletion (g.482+82_856-854del) in IL12B. This IL12-deficient child suffered from infections caused by bacille Calmette-Guérin (BCG) and Salmonella enteritidis. We herein report 12 additional patients from five other kindreds. In one kindred from India, the same large deletion that was described elsewhere (g.482+82_856-854del) was identified. In four kindreds from Saudi Arabia, a recessive loss-of-function frameshift insertion (g.315_316insA) was found. A conserved haplotype encompassing the IL12B gene suggested that a founder effect accounted for the recurrence of each mutation. The two founder mutational events-g.482+82_856-854del and g.315_316insA-were estimated to have occurred approximately 700 and approximately 1,100 years ago, respectively. Among a total of 13 patients with IL12 deficiency, 1 child had salmonellosis only and 12 suffered from clinical disease due to BCG or environmental nontuberculous mycobacteria. One patient also had clinical disease caused by virulent Mycobacterium tuberculosis, five patients had clinical disease caused by Salmonella serotypes, and one patient had clinical disease caused by Nocardia asteroides. The clinical outcome varies from case to case, since five patients (aged 2-11 years) died of overwhelming infection, whereas eight patients (aged 3-12 years) are still in good health and are not currently taking antibiotics. In conclusion, IL12 deficiency is not limited to a single kindred, shows significant variability of outcome, and should be considered in the genetic diagnosis of patients with mycobacteriosis and/or salmonellosis. To date, two founder IL12B mutations have been identified, accounting for the recurrence of a large deletion and a small insertion within populations from the Indian subcontinent and from the Arabian Peninsula, respectively.
白细胞介素-12(IL12)是一种由活化的吞噬细胞和树突状细胞分泌的细胞因子,可诱导自然杀伤细胞和T淋巴细胞产生γ干扰素。它由两个亚基p35和p40组成,分别由IL12A和IL12B编码。首例报道的患有遗传性细胞因子疾病的患者是一名巴基斯坦儿童,其IL12B基因存在一个导致功能大幅丧失的大片段缺失(g.482 + 82_856 - 854del)的纯合子。这名IL12缺陷儿童患有由卡介苗(BCG)和肠炎沙门氏菌引起的感染。我们在此报告来自其他五个家族的另外12名患者。在一个来自印度的家族中,发现了与其他地方描述相同的大片段缺失(g.482 + 82_856 - 854del)。在来自沙特阿拉伯的四个家族中,发现了一种隐性功能丧失的移码插入(g.315_316insA)。一个包含IL12B基因的保守单倍型表明,奠基者效应导致了每个突变的复发。这两个奠基者突变事件——g.482 + 82_856 - 854del和g.315_316insA——估计分别发生在大约700年前和大约1100年前。在总共13名IL12缺陷患者中,1名儿童仅患有沙门氏菌病,12名患者因卡介苗或环境非结核分枝杆菌而患有临床疾病。1名患者还患有由强毒结核分枝杆菌引起的临床疾病,5名患者患有由沙门氏菌血清型引起的临床疾病,1名患者患有由星形诺卡菌引起的临床疾病。临床结果因病例而异,因为5名患者(年龄在2至11岁之间)死于严重感染,而8名患者(年龄在3至12岁之间)仍健康良好,目前未服用抗生素。总之,IL12缺陷并不局限于单个家族,显示出显著的结果变异性,在分枝杆菌病和/或沙门氏菌病患者的基因诊断中应予以考虑。迄今为止,已鉴定出两种奠基者IL12B突变,分别解释了印度次大陆人群和阿拉伯半岛人群中大片段缺失和小插入的复发情况。
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