Abstract
Kashin-Beck disease, a syndrome characterized by short stature, skeletal deformities, and arthropathy of multiple joints, is highly prevalent in specific regions of Asia. The disease has been postulated to result from a combination of different environmental factors, including contamination of barley by mold mycotoxins, iodine deficiency, presence of humic substances in drinking water, and, importantly, deficiency of selenium. This multifunctional trace element, in the form of selenocysteine, is essential for normal selenoprotein function, including attenuation of excessive oxidative stress, and for the control of redox-sensitive molecules involved in cell growth and differentiation. To investigate the effects of skeletal selenoprotein deficiency, a Cre recombinase transgenic mouse line was used to trigger Trsp gene deletions in osteo-chondroprogenitors. Trsp encodes selenocysteine tRNA[Ser]Sec, required for the incorporation of selenocysteine residues into selenoproteins. The mutant mice exhibited growth retardation, epiphyseal growth plate abnormalities, and delayed skeletal ossification, as well as marked chondronecrosis of articular, auricular, and tracheal cartilages. Phenotypically, the mice thus replicated a number of the pathological features of Kashin-Beck disease, supporting the notion that selenium deficiency is important to the development of this syndrome.
Highlights
Kashin-Beck disease, an environmentally-induced musculoskeletal syndrome, is prevalent in millions of individuals residing within specific regions of Tibet, China, Siberia, and North Korea [1,2,3]
The disease first becomes evident in childhood with affected individuals exhibiting short stature, joint and limb deformities, and radiographic evidence of delayed skeletal ossification [4,5]; features attributed to impaired epiphyseal growth and chondronecrosis [1,3,4,6]
UGA specifies a ‘stop’ codon in the universal genetic code, it can code for Sec with the participation of a group of proteins that recognize the Sec insertion sequence (SECIS) element located in the 39 untranslated region of selenoprotein mRNAs [14]
Summary
Kashin-Beck disease, an environmentally-induced musculoskeletal syndrome, is prevalent in millions of individuals residing within specific regions of Tibet, China, Siberia, and North Korea [1,2,3]. Several factors have been implicated in the pathogenesis of this disease, deficiency of dietary selenium intake, and profoundly low serum selenium levels represent one of the most salient features of Kashin-Beck disease [1,7,8]. This raised the possibility that deficiencies in one or more selenoproteins might play key etiological roles in this musculoskeletal disorder. UGA is recognized by Sec tRNA (designated Sec tRNA[Ser]Sec) which is encoded by Trsp (present in one copy per haploid genome)
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