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Journal of Assisted Reproduction and Genetics

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Open Access 01-03-2019 | Commentary

Overcoming bioethical, legal, and hereditary barriers to mitochondrial replacement therapy in the USA

Authors: Marybeth Pompei, Francesco Pompei

Published in: Journal of Assisted Reproduction and Genetics | Issue 3/2019

Abstract

The purpose of the paper is to explore novel means to overcome the controversial ban in the USA against mitochondrial replacement therapy, a form of IVF, with the added step of replacing a woman’s diseased mutated mitochondria with a donor’s healthy mitochondria to prevent debilitating and often fatal mitochondrial diseases. Long proven effective in non-human species, MRT recently performed in Mexico resulted in the birth of a healthy baby boy. We explore the ethics of the ban, the concerns over hereditability of mitochondrial disease and its mathematical basis, the overlooked role of Mitochondrial Eve, the financial burden of mitochondrial diseases for taxpayers, and a woman’s reproductive rights. We examine applicable court cases, particularly protection of autonomy within the reproductive rights assured by Roe v Wade. We examine the consequences of misinterpreting MRT as genetic engineering in the congressional funding prohibitions causing the MRT ban by the FDA. Allowing MRT to take place in the USA would ensure a high standard of reproductive medicine and safety for afflicted women wishing to have genetically related children, concurrently alleviating the significant financial burden of mitochondrial diseases on its taxpayers. Since MRT does not modify any genome, it falls outside the “heritable genetic modification” terminology of concern to Congress and the FDA. Correcting this terminology, the IOM’s conclusion that MRT is ethical, the continuing normalcy of the first MRT recipient, and increasing public awareness of the promising benefits might be all that is required to modify the FDA’s position on MRT.

To estimate the distribution of total offspring per woman, we used data from women at early post-reproductive ages. For US women age 45–50, year 2016 data are available on offspring per woman [85] and the overall offspring sex ratio [86]. Sex-specific offspring distributions were obtained from these data by assuming sex ratio is independent of offspring numbers, which likely holds approximately but not exactly.

To investigate the number of generations from mtDNA transplantation to a female recipient until extinction of the new mtDNA line, we simulated one million runs of the Galton-Watson process with offspring distributions taken from the year 2016 US data. Each run of the simulation was adjusted for the possibility that there could be a final, male only generation of carriers of the new mtDNA line.

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Title: Overcoming bioethical, legal, and hereditary barriers to mitochondrial replacement therapy in the USA
Authors: Marybeth Pompei
Francesco Pompei
Publication date: 01-03-2019
Publisher: Springer US
Published in: Journal of Assisted Reproduction and Genetics / Issue 3/2019
Print ISSN: 1058-0468
Electronic ISSN: 1573-7330
DOI: https://doi.org/10.1007/s10815-018-1370-7

Keynote webinar | Spotlight on medication adherence

Springer Medicine

Overcoming bioethical, legal, and hereditary barriers to mitochondrial replacement therapy in the USA

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Keynote webinar | Spotlight on medication adherence

Springer Medicine

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