Although research is ongoing, treatment options are currently limited;
vitamins are frequently prescribed, though the evidence for their effectiveness is limited.
Pyruvate has been proposed in 2007 as a treatment option.
N-acetyl cysteine reverses many models of mitochondrial dysfunction.
Mood disorders In the case of mood disorders, specifically
bipolar disorder, it is hypothesized that
N-acetyl-cysteine (NAC),
acetyl-L-carnitine (ALCAR),
S-adenosylmethionine (SAMe),
coenzyme Q10 (CoQ10),
alpha-lipoic acid (ALA),
creatine monohydrate (CM), and
melatonin could be potential treatment options. Using a similar
pronuclear transfer technique, researchers at
Newcastle University led by
Douglass Turnbull successfully transplanted healthy DNA in human eggs from women with mitochondrial disease into the eggs of women donors who were unaffected. In such cases, ethical questions have been raised regarding biological motherhood, since the child receives genes and gene regulatory molecules
from two different women. Using genetic engineering in attempts to produce babies free of mitochondrial disease is controversial in some circles and raises important
ethical issues. A male baby was born in Mexico in 2016 from a mother with Leigh syndrome using MRT. In September 2012 a public consultation was launched in the UK to explore the ethical issues involved. Human genetic engineering was used on a small scale to allow infertile women with genetic defects in their
mitochondria to have children. In June 2013, the
United Kingdom government agreed to develop legislation that would legalize the 'three-person
IVF' procedure as a treatment to fix or eliminate mitochondrial diseases that are passed on from mother to child. The procedure could be offered from 29 October 2015 once regulations had been established.
Embryonic mitochondrial transplant and
protofection have been proposed as a possible treatment for inherited mitochondrial disease, and
allotopic expression of mitochondrial proteins as a radical treatment for mtDNA mutation load. In June 2018 Australian Senate's Senate Community Affairs References Committee recommended a move towards legalising MRT. Research and clinical applications of MRT were overseen by laws made by federal and state governments. State laws were, for the most part, consistent with federal law. In all states, legislation prohibited the use of MRT techniques in the clinic, and except for Western Australia, research on a limited range of MRT was permissible up to day 14 of embryo development, subject to a license being granted. In 2010, the Hon. Mark Butler MP, then Federal Minister for Mental Health and Ageing, had appointed an independent committee to review the two relevant acts: the
Prohibition of Human Cloning for Reproduction Act 2002 and the
Research Involving Human Embryos Act 2002. The committee's report, released in July 2011, recommended the existing legislation remain unchanged Currently, human clinical trials are underway at GenSight Biologics (ClinicalTrials.gov # NCT02064569) and the University of Miami (ClinicalTrials.gov # NCT02161380) to examine the safety and efficacy of mitochondrial gene therapy in Leber's hereditary optic neuropathy. ==Epidemiology==