Abstract
Melanin pigment helps protect our body from broad wavelength solar radiation and skin cancer. Among other pigmentation disorders in humans, albinism is reported to manifest in both syndromic and nonsyndromic forms as well as with varying inheritance patterns. Oculocutaneous albinism (OCA), an autosomal recessive nonsyndromic form of albinism, presents as partial to complete loss of melanin in the skin, hair, and iris. OCA has been known to be caused by pathogenic variants in seven different genes, so far, according to all the currently published population studies. However, the detection rate of alleles causing OCA varies from 50% to 90%. One of the significant challenges of uncovering the pathological variant underlying disease etiology is inter- and intra-familial locus heterogeneity. This problem is especially pertinent in highly inbred populations. As examples of such familial locus heterogeneity, we present nine consanguineous Pakistani families with segregating OCA due to variants in one or two different known albinism-associated genes. All of the identified variants are predicted to be pathogenic, which was corroborated by several in silico algorithms and association with diverse clinical phenotypes. We report an individual affected with OCA carries heterozygous, likely pathogenic variants in TYR and OCA2, raising the question of a possible digenic inheritance. Altogether, our study highlights the significance of exome sequencing for the complete genetic diagnosis of inbred families and provides the ramifications of potential genetic interaction and digenic inheritance of variants in the TYR and OCA2 genes.
Highlights
Melanosomes are the cellular organelles (~500 nm in diameter) that are involved in the synthesis, storage, and transportation of melanin pigment in various tissues
Slit lamp microscopy in the affected individuals (IV:1 and IV:2) of family PKAB107 showed iris transillumination and albinotic fundus (Figure 3C) that is consistent with the albinism phenotype
Oculocutaneous albinism (OCA) is a clinically and genetically heterogeneous disorder that segregates in an autosomal recessive pattern in humans
Summary
Melanosomes are the cellular organelles (~500 nm in diameter) that are involved in the synthesis, storage, and transportation of melanin pigment in various tissues. This includes but is not limited to the skin, retinal pigment epithelium cells (RPE), and stria vascularis of the inner ear in mammals [1]. Significant aberrations at any stage of melanocyte, melanosome, or melanin synthesis and their inter- and intracellular transport can lead to heterogeneous pigmentation disorders in humans. Oculocutaneous albinism (OCA) is a pigmentation disorder that presents a lack of pigment in the skin, eyes, and hair follicles [7]. In humans, OCA can manifest as part of a multi-organ syndrome or an isolated (non-syndromic; nsOCA) clinical entity
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