Washington: A new study discovered that the SMCHD1 protein controls how genes are digested, which influences the course of Facioscapulohumeral Muscular Dystrophy (FSHD). This finding about SMCHD1’s role in gene regulation is significant because it offers up new avenues for creating tailored therapeutic techniques to combat the disease. Scientists can discover new approaches to combat the disease if they learn more about how SMCHD1 functions.

A recent study by MD-PhD student Eden Engal, led by Dr Yotam Drier and Prof. Maayan Salton from Hebrew University‘s Faculty of Medicine, highlighted the critical role of the SMCHD1 protein in the regulation of alternative splicing, shedding light on the development of Facioscapulohumeral Muscular Dystrophy (FSHD). Genetic factors drive this complex condition that causes increasing muscular weakness and loss of function. The team’s results improve our understanding of the genetic pathways that cause this devastating illness.

FSHD is one of the most common forms of muscular dystrophy, affecting approximately 1 in 20,000 people worldwide. It is caused by genetic mutations that lead to the inappropriate activation of the DUX4 gene in muscle cells and this activation disrupts normal muscle function and causes muscle cells to deteriorate over time. The severity of the disease can vary widely, with some individuals experiencing mild symptoms while others may lose significant muscle function and mobility. There is currently no cure for FSHD.

As DNA is transcribed into RNA, parts of the genes are removed from the RNA in a process known as splicing. Which parts are removed is regulated by multiple proteins and can lead to production of different proteins from the same DNA, a phenomenon therefore termed alternative splicing.

The new study found that in addition to SMCHD1 known role in regulating chromosome structure, it is also strongly affecting alternative splicing. Mutations in the SMCHD1 gene were already known to lead to DUX4 expression and FSHD, but it was not clear how.

A detailed analysis of RNA sequencing data from muscle biopsies of FSHD patients and cells genetically modified to lack SMCHD1 revealed extensive splicing errors in numerous genes due to the absence of SMCHD1. A comprehensive screening of splicing factors identified the involvement of the splicing factor RBM5 in these anomalies, and further experiments confirmed that SMCHD1 is required for recruiting RBM5 to its target RNA sites.

Amongst the genes whose splicing was disrupted, the researchers identified the DNMT3B gene. They have then demonstrated that the changes in DNMT3B splicing lead to reduced DNA methylation at specific sites near DUX4 which in turn cause harmful overexpression of the DUX4 gene, significantly contributing to FSHD development.

“Our findings underscore a vital link between SMCHD1 and the regulation of splicing mechanisms that, when disrupted, activate pathological processes in Facioscapulohumeral Muscular Dystrophy,” stated Eden Engal. “This understanding opens new avenues for potential therapeutic strategies that target these splicing errors, offering hope for mitigating the disease’s progression.”

  • Published On Jun 5, 2024 at 10:30 AM IST

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