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Safe Way to Conduct Mitochondrial Replacement Therapy

by Dr. Meenakshy Varier on December 1, 2016 at 4:49 PM
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Highlights

Mitochondria are tiny powerhouses inside cells in the human body.


Mothers pass the mitochondrial DNA to their children. During this transfer, children might also inherit harmful mutations from mothers. These mutations can cause potentially fatal disorders affecting organs like heart, muscles and brain.

‘Careful selection of donor during mitochondrial replacement therapy is imperative to prevent transmission of harmful mutations.’

Mitochondrial replacement therapy is a new gene therapy that involves replacing the faulty mitochondria with those from a healthy donor. It offers hope for women who are genetically predisposed to pass on mutant mitochondria.

Mitochondrial replacement therapy has been approved for clinical trials in the United Kingdom.

Similar group of mitochondrial DNA are known as halotypes. Each halotypes represent major branching points on the human genetic family tree.

Researchers led by Shoukhrat Mitalipov, Ph.D. are studying how to conduct mitochondrial replacement therapy in a safe way to prevent the transmission of harmful mutant mitochondrial DNA from mothers to children.

"This research suggests that we're going to have the greatest success rates for producing an embryo free of disease-causing genetic mutations by making sure we are using the right combination of haplotypes," said senior author Shoukhrat Mitalipov, Ph.D., who directs the Center for Embryonic Cell and Gene Therapy at OHSU.

The study published in the Nature suggest how clinicians select egg donors whose mitochondrial DNA (mtDNA) is compatible with the mother's ancestral mitochondria.

Spindle-Transfer Technique

Shoukhrat Mitalipov had previously pioneered the spindle-transfer technique. This technique involves transferring the nucleus - or spindle - of a mother's egg into a donor egg stripped of its nucleus.

This technique has a small glitch as even a small amount of mutant mitochondrial DNA transferred with the mother's nucleus can replicate quickly as the embryo develops and cause the disease.

Choosing Healthy Donors

For the current research, Mitalipov and colleagues recruited four families who have children suffering from Leigh Syndrome and one with a neurodegenerative disorder called MELAS.

Donor eggs from 11 healthy women were collected and screened to confirm that they did not carry inherited pathogenic mutations in their mtDNA.

Spindles from carrier eggs were transferred into 36 donor eggs stripped of their nuclei. They were fertilized, cultured to blastocysts, and subsequently to embryonic stem cell lines.

Most stem cells developed with the donor's healthy mitochondrial DNA continuing to dominate.

But a few stem cell lines displayed gradual return to the mutant maternal mtDNA. As those stem cell lines continued to grow in the laboratory, they reverted completely to the original maternal mitochondrial DNA.

The Reason for Reverting to Mutant Maternal mtDNA-

"Currently, there is a lack of studies on the efficacy and safety of oocytes derived from women carrying pathogenic mtDNA mutations," said co-author Juan Carlos Izpisua Belmonte, Ph.D., with the Salk Institute for Biological Studies in La Jolla, California. "Our study fills the gap."

When researchers identified a portion of the mtDNA known as the D-loop, which initiates replication of the entire genetic sequence, they discovered DNA code polymorphisms that result in preferential replication of the mother's mtDNA.

In order to conduct mitochondrial replacement therapy at clinical levels, researchers are proposing careful selection of donor mitochondria to avoid a return of mutant mitochondria.

Source: Medindia

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