Abstract
The gene encoding the cytosolic β-glucosidase GBA3 shows pseudogenization due to a truncated allele (rs358231) that is polymorphic in humans. Since this enzyme is involved in the transformation of many plant β-glycosides, this particular case of gene loss may have been influenced by dietary adaptations during evolution. In humans, apart from the inactivating allele, we found that GBA3 accumulated additional damaging mutations, implying an extensive GBA3 loss. The allelic distribution of loss-of-function alleles revealed significant differences between human populations which can be partially related with their staple diet. The analysis of mammalian orthologs disclosed that GBA3 underwent at least nine pseudogenization events. Most events of pseudogenization occurred in carnivorous lineages, suggesting a possible link to a β-glycoside poor diet. However, GBA3 was also lost in omnivorous and herbivorous species, hinting that the physiological role of GBA3 is not fully understood and other unknown causes may underlie GBA3 pseudogenization. Such possibility relies upon a putative role in sialic acid biology, where GBA3 participates in a cellular network involving NEU2 and CMAH. Overall, our data shows that the recurrent loss of GBA3 in mammals is likely to represent an evolutionary endpoint of the relaxation of selective constraints triggered by diet-related factors.
Highlights
The gene encoding the cytosolic β-glucosidase GBA3 shows pseudogenization due to a truncated allele that is polymorphic in humans
A classic example of neutral gene loss in humans and other mammals is the inactivation of the gene encoding L-gulonolactone oxidase (GULO), the enzyme catalysing the final step in vitamin C biosynthesis, whose loss has been attributed to dietary compensation in lineages where the diet provides a steady source of ascorbic a cid[3,4]
The elucidation of the still obscure physiological function of GBA3 has been greatly hindered by the lack of knowledge on any specific endogenous substrate of the enzyme, as well as by the fact that the loss of its functionality does not result in any phenotypic consequences recognized up to n ow[18]
Summary
The gene encoding the cytosolic β-glucosidase GBA3 shows pseudogenization due to a truncated allele (rs358231) that is polymorphic in humans. Since this enzyme is involved in the transformation of many plant β-glycosides, this particular case of gene loss may have been influenced by dietary adaptations during evolution. While one of the counterparts retains its primordial function, the other can experience different fates, including pseudogenization (i.e. gene silencing by the accumulation of disruptive mutations) which is the most common outcome for the redundant c opy[2]. Due to the similarity with GBA, GBA3 was initially hypothesized to act as a modifier in Gaucher d isease[16,18], but yet a study focusing the issue did not succeed to find any evidence sustaining the relationship and even revealed that the GBA3 presented low activity towards the substrates of GBA18
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