Scientists May Have Found A Genomic Off Switch For Down’s Syndrome

Scientists May Have Found A Genomic Off Switch For Down’s Syndrome

One in every thousand or so babies born today will suffer from Down Syndrome, a genetic disorder caused by the presence of a third copy of chromosome 21 that results in learning disabilities, a heightened risk of bowel and blood diseases, and a severely heightened risk of dementia later in life. But a radical new genome treatment method could hold the key to turning off that extra chromosome 21 like a light.

Normally, every human carries 23 chromosome pairs which provide the genetic blueprint by which the body operates during its life. However, people with DS have either a partial or full extra copy of chromosome 21. This superfluous genetic data causes the symptoms commonly associated with the disease. However, a team of researchers from the University of Massachusetts led by Dr. Jeanne Lawrence have just published some exciting study results in the journal Nature suggesting a potent new treatment method for DS.

The UMass team employed a technique known as “genome editing” to inject the XIST gene into the extra chromosome of cells cultured from DS patients. XIST is a gene vital to embryonic development. It plays a major role in gender determination by silencing the second X chromosome thereby turning the foetus male (if it doesn’t turn on, the second X chromosome remains active and the baby will be female). It’s this genomic silencing ability that Lawrence’s team exploited against chromosome 21.

After inserting XIST into the extra chromosome, the body coats and smothers it with RNA, effectively turning the chromosome off and halting the effects of its expressed genes. Individual cell cultures treated with this technique showed stronger, faster growth. Lawrence’s team hopes that this breakthrough will someday help alleviate the early-onset dementia that some 60 per cent of DS patients suffer from by the time they hit 60 years. It could potentially — and the possibility is very remote at this point — eliminate the disease entirely through a prenatal gene therapy.

What’s more, the technique has already shown promise with other similar diseases such as Lawrence explained to The Guardian. “But that is 10 years or more away. I don’t want to get people’s hopes up.”

So before the medical community begins tinkering with people’s genetic code, much more research has to be done. The next step is mouse model trials; injecting the XIST into early-stage embryonic mice to correct their cells. Beyond that, the research could hit a stumbling block in the ethical dilemma of whether or not to experiment on in vitro humans. On the other hand, 10 years is a long time and, given the rapid advancements of artificial cell organelles, we may be able to sidestep human experimentation altogether. [Guardian]

Picture: Denis Kuvaev / Shutterstock


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