University of Toronto, Toronto, ON, Canada.
Universidade de Campinas, Campinas, SP, Brazil.
Rev Paul Pediatr. 2021 Oct 29;40:e2020434. doi: 10.1590/1984-0462/2022/40/2020434. eCollection 2021.
To report two patients with very-early-onset inflammatory bowel disease (VEOIBD) secondary to interleukin-10 receptor (IL-10R) mutations, explore immunophenotyping data and plasma cytokine profile on these cases compared to healthy controls, and describe the phenotype of IL-10/IL-10R mutations based on a literature review.
We report on two female infants referred to our tertiary center at the age of ten months, with severe colonic and perianal disease, as well as significant malnutrition, who had shown limited response to usual inflammatory bowel disease (IBD) therapy agents. In the first case, whole-exome sequencing (WES) revealed a homozygous (c.537G>A/p.T179T) mutation in exon 4 of the IL-10RA gene, while in the second patient, compound heterozygosity was identified, also in the IL-10RA gene (chr11:117.859.199 variant A>G/p.Tyr57Cys and chr11: 117.860.335 variant G>T/p.Val123Leu). Both patients underwent hematopoietic cell transplantation (HCT). Immunological work-up of these patients revealed increased IL-10 plasma levels and increased IgA.
Our case reports disclose novel findings on plasma cytokine profile in IL-10R deficiency, and we describe the severe phenotype of IL-10/IL-10R deficiency that should be recognized by physicians.
报告两例由白细胞介素-10 受体(IL-10R)突变引起的非常早发性炎症性肠病(VEOIBD)患者,探讨这些病例与健康对照相比的免疫表型数据和血浆细胞因子谱,并基于文献复习描述 IL-10/IL-10R 突变的表型。
我们报告了两名女性婴儿,在十个月大时因严重的结肠和肛周疾病以及严重的营养不良而被转诊至我们的三级中心,她们对常规炎症性肠病(IBD)治疗药物的反应有限。在第一个病例中,全外显子组测序(WES)显示 IL-10RA 基因外显子 4 中的纯合突变(c.537G>A/p.T179T),而在第二个病例中,鉴定出复合杂合突变,同样在 IL-10RA 基因中(chr11:117.859.199 变异 A>G/p.Tyr57Cys 和 chr11:117.860.335 变异 G>T/p.Val123Leu)。这两名患者均接受了造血细胞移植(HCT)。对这些患者进行的免疫检查发现,IL-10R 缺陷患者的血浆细胞因子谱中 IL-10 水平升高,IgA 升高。
我们的病例报告揭示了 IL-10R 缺陷患者血浆细胞因子谱的新发现,并描述了 IL-10/IL-10R 缺陷的严重表型,医生应予以识别。
