Department of Cytogenetics, National Institute of Immunohaematology (ICMR), 13th floor, new multistoried building, K.E.M Hospital campus, Parel, Mumbai, 400012, India.
BMC Med Genomics. 2022 Jan 3;15(1):2. doi: 10.1186/s12920-021-01152-1.
Oculocutaneous albinism (OCA) is an autosomal recessive disorder characterized by hypo-pigmentation of skin, hair, and eyes. The OCA clinical presentation is due to a deficiency of melanin biosynthesis. Intellectual disability (ID) in OCA cases is a rare clinical presentation and appropriate diagnosis of ID is challenging through clinical examination. We report an Indian family with a rare co-inheritance of OCA1B and ID due to a novel TYR gene variant and chromosomal copy number variations.
We have done a study on three siblings (2 males and 1 female) of a family where all of them presented with hypopigmented skin, hair and eyes. The male children and their father was affected with ID. Targeted exome sequencing and multiplex ligation-dependent probe amplification analysis were carried out to identify the OCA1B and ID associated genomic changes. Further Array-CGH was performed using SurePrint G3 Human CGH + SNP, 8*60 K array.
A rare homozygous deletion of exon 3 in TYR gene causing OCA1B was identified in all three children. The parents were found to be heterozygous carriers. The Array-CGH analysis revealed paternally inherited heterozygous deletion(1.9 MB) of 15q11.1-> 15q11.2 region in all three children. Additionally, paternally inherited heterozygous deletion(2.6 MB)of 10q23.2-> 10q23.31 region was identified in the first male child; this may be associated with ID as the father and the child both presented with ID. While the 2nd male child had a denovo duplication of 13q31.1-> 13q31.3 chromosomal region.
A rare homozygous TYR gene exon 3 deletion in the present study is the cause of OCA1B in all three children, and the additional copy number variations are associated with the ID. The study highlights the importance of combinational genetic approaches for diagnosing two different co-inherited disorders (OCA and ID). Hence, OCA cases with additional clinical presentation need to be studied in-depth forthe appropriate management of the disease.
眼皮肤白化病(OCA)是一种常染色体隐性疾病,其特征为皮肤、毛发和眼睛色素减退。OCA 的临床表现是由于黑色素生物合成缺陷所致。OCA 病例中的智力障碍(ID)是一种罕见的临床表现,通过临床检查对 ID 进行准确诊断具有挑战性。我们报告了一个印度家庭,由于 TYR 基因的一个新变异和染色体拷贝数变异,同时遗传了 OCA1B 和 ID。
我们对一个家庭的三个兄弟姐妹(2 男 1 女)进行了研究,他们均表现出皮肤、毛发和眼睛色素减退。两个男孩及其父亲患有 ID。进行靶向外显子组测序和多重连接依赖性探针扩增分析,以鉴定与 OCA1B 和 ID 相关的基因组变化。进一步使用 SurePrint G3 Human CGH + SNP,8*60 K 阵列进行了微阵列比较基因组杂交分析。
在所有三个孩子中均发现 TYR 基因exon 3 的罕见纯合缺失,导致 OCA1B。父母被发现为杂合携带者。Array-CGH 分析显示,所有三个孩子均存在父系遗传的 15q11.1-> 15q11.2 区域杂合缺失(1.9 MB)。此外,在第一个男孩中还发现了父系遗传的杂合缺失(2.6 MB)10q23.2-> 10q23.31 区域,这可能与 ID 相关,因为父亲和孩子均患有 ID。而第二个男孩则出现了 13q31.1-> 13q31.3 染色体区域的新发重复。
本研究中,三个孩子均存在罕见的 TYR 基因 exon 3 纯合缺失,导致 OCA1B,此外还存在额外的拷贝数变异,与 ID 相关。该研究强调了组合遗传方法在诊断两种不同的共遗传疾病(OCA 和 ID)中的重要性。因此,需要对伴有其他临床表现的 OCA 病例进行深入研究,以进行适当的疾病管理。
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