Rapamycin prevents, but does not reverse, aberrant migration in Pten knockout neurons

Stephanie A. Getz; Tyrone DeSpenza, Jr; Meijie Li; Bryan W. Luikart

Neurobiology of Disease (Sep 2016)

Rapamycin prevents, but does not reverse, aberrant migration in Pten knockout neurons

Stephanie A. Getz,
Tyrone DeSpenza, Jr,
Meijie Li,
Bryan W. Luikart

Affiliations

Stephanie A. Getz: Department of Physiology and Neurobiology, Geisel School of Medicine at Dartmouth College Lebanon, NH 03756, United States
Tyrone DeSpenza, Jr: Department of Physiology and Neurobiology, Geisel School of Medicine at Dartmouth College Lebanon, NH 03756, United States
Meijie Li: Department of Physiology and Neurobiology, Geisel School of Medicine at Dartmouth College Lebanon, NH 03756, United States
Bryan W. Luikart: Corresponding author at: Geisel School of Medicine at Dartmouth, Physiology and Neurobiology, 1 Medical Center Drive, Borwell 708E, Lebanon 03756, United States.; Department of Physiology and Neurobiology, Geisel School of Medicine at Dartmouth College Lebanon, NH 03756, United States

Journal volume & issue: Vol. 93
pp. 12 – 20

Abstract

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Phosphatase and tensin homolog (PTEN) is a major negative regulator of the Akt/mammalian target of rapamycin (MTOR) pathway. Mutations in PTEN have been found in a subset of individuals with autism and macrocephaly. Further, focal cortical dysplasia (FCD) has been observed in patients with PTEN mutations prompting us to examine the role of Pten in neuronal migration. The dentate gyrus of PtenFlox/Flox mice was injected with Cre- and non-Cre-expressing retroviral particles, which integrate into the dividing genome to birthdate cells. Control and Pten knockout (KO) cell position in the granule cell layer was quantified over time to reveal that Pten KO neurons exhibit an aberrant migratory phenotype beginning at 7.5 days-post retroviral injection (DPI). We then assessed whether rapamycin, a mTor inhibitor, could prevent or reverse aberrant migration of granule cells. The preventative group received daily intraperitoneal (IP) injections of rapamycin from 3 to 14 DPI, before discrepancies in cell position have been established, while the reversal group received rapamycin afterward, from 14 to 24 DPI. We found that rapamycin prevented and reversed somal hypertrophy. However, rapamycin prevented, but did not reverse aberrant migration in Pten KO cells. We also find that altered migration occurs through mTorC1 and not mTorC2 activity. Together, these findings suggest a temporal window by which rapamycin can treat aberrant migration, and may have implications for the use of rapamycin to treat PTEN-mutation associated disorders. Significance statement: Mutations in phosphatase and tensin homolog (PTEN) have been linked to a subset of individuals with autism and macrocephaly, as well as Cowden Syndrome and focal cortical dysplasia. Pten loss leads to neuronal hypertrophy, but the role of Pten in neuronal migration is unclear. Here we have shown that loss of Pten leads to aberrant migration, which can be prevented but not reversed by treatment with rapamycin, a mTor inhibitor. These results are important to consider as clinical trials are developed to examine rapamycin as a therapeutic for autism with PTEN mutations. Our findings show that some abnormalities cannot be reversed, and suggest the potential need for genetic screening and preventative treatment.

Published in Neurobiology of Disease

ISSN: 0969-9961 (Print); 1095-953X (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry
Website: https://www.journals.elsevier.com/neurobiology-of-disease

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