Gorlin syndrome-derived induced pluripotent stem cells are hypersensitive to hedgehog-mediated osteogenic induction

Gorlin syndrome is an autosomal dominant inherited syndrome that predisposes a patient to the formation of basal cell carcinomas, odontogenic keratocysts, and skeletal anomalies. Causative mutations in several genes associated with the sonic hedgehog (SHH) signaling pathway, including PTCH1, have be...

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Autores principales: Hasegawa, Daigo, Ochiai-Shino, Hiromi, Onodera, Shoko, Nakamura, Takashi, Saito, Akiko, Onda, Takeshi, Watanabe, Katsuhito, Nishimura, Ken, Ohtaka, Manami, Nakanishi, Mahito, Kosaki, Kenjiro, Yamaguchi, Akira, Shibahara, Takahiko, Azuma, Toshifumi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5663396/
https://www.ncbi.nlm.nih.gov/pubmed/29088246
http://dx.doi.org/10.1371/journal.pone.0186879
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author Hasegawa, Daigo
Ochiai-Shino, Hiromi
Onodera, Shoko
Nakamura, Takashi
Saito, Akiko
Onda, Takeshi
Watanabe, Katsuhito
Nishimura, Ken
Ohtaka, Manami
Nakanishi, Mahito
Kosaki, Kenjiro
Yamaguchi, Akira
Shibahara, Takahiko
Azuma, Toshifumi
author_facet Hasegawa, Daigo
Ochiai-Shino, Hiromi
Onodera, Shoko
Nakamura, Takashi
Saito, Akiko
Onda, Takeshi
Watanabe, Katsuhito
Nishimura, Ken
Ohtaka, Manami
Nakanishi, Mahito
Kosaki, Kenjiro
Yamaguchi, Akira
Shibahara, Takahiko
Azuma, Toshifumi
author_sort Hasegawa, Daigo
collection PubMed
description Gorlin syndrome is an autosomal dominant inherited syndrome that predisposes a patient to the formation of basal cell carcinomas, odontogenic keratocysts, and skeletal anomalies. Causative mutations in several genes associated with the sonic hedgehog (SHH) signaling pathway, including PTCH1, have been identified in Gorlin syndrome patients. However, no definitive genotype—phenotype correlations are evident in these patients, and their clinical presentation varies greatly, often leading to delayed diagnosis and treatment. We generated iPSCs from four unrelated Gorlin syndrome patients with loss-of-function mutations in PTCH1 using the Sendai virus vector (SeVdp(KOSM)302). The patient-derived iPSCs exhibited basic iPSC features, including stem cell marker expression, totipotency, and the ability to form teratomas. GLI1 expression levels were greater in fibroblasts and patient-derived iPSCs than in the corresponding control cells. Patient-derived iPSCs expressed lower basal levels than control iPSCs of the genes encoding the Hh ligands Indian Hedgehog (IHH) and SHH, the Hh acetyltransferase HHAT, Wnt proteins, BMP4, and BMP6. Most of these genes were upregulated in patient-derived iPSCs grown in osteoblast differentiation medium (OBM) and downregulated in control iPSCs cultured in OBM. The expression of GLI1 and GLI2 substantially decreased in both control and patient-derived iPSCs cultured in OBM, whereas GLI3, SHH, and IHH were upregulated in patient-derived iPSCs and downregulated in control iPSCs grown in OBM. Activation of Smoothened by SAG in cells grown in OBM significantly enhanced alkaline phosphatase activity in patient-derived iPSCs compared with control iPSC lines. In summary, patient-derived iPSCs expressed lower basal levels than the control iPSCs of the genes encoding Hh, Wnt, and bone morphogenetic proteins, but their expression of these genes strongly increased under osteogenic conditions. These findings indicate that patient-derived iPSCs are hypersensitive to osteogenic induction. We propose that Hh signaling is constituently active in iPSCs from Gorlin syndrome patients, enhancing their response to osteogenic induction and contributing to disease-associated abnormalities.
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spelling pubmed-56633962017-11-09 Gorlin syndrome-derived induced pluripotent stem cells are hypersensitive to hedgehog-mediated osteogenic induction Hasegawa, Daigo Ochiai-Shino, Hiromi Onodera, Shoko Nakamura, Takashi Saito, Akiko Onda, Takeshi Watanabe, Katsuhito Nishimura, Ken Ohtaka, Manami Nakanishi, Mahito Kosaki, Kenjiro Yamaguchi, Akira Shibahara, Takahiko Azuma, Toshifumi PLoS One Research Article Gorlin syndrome is an autosomal dominant inherited syndrome that predisposes a patient to the formation of basal cell carcinomas, odontogenic keratocysts, and skeletal anomalies. Causative mutations in several genes associated with the sonic hedgehog (SHH) signaling pathway, including PTCH1, have been identified in Gorlin syndrome patients. However, no definitive genotype—phenotype correlations are evident in these patients, and their clinical presentation varies greatly, often leading to delayed diagnosis and treatment. We generated iPSCs from four unrelated Gorlin syndrome patients with loss-of-function mutations in PTCH1 using the Sendai virus vector (SeVdp(KOSM)302). The patient-derived iPSCs exhibited basic iPSC features, including stem cell marker expression, totipotency, and the ability to form teratomas. GLI1 expression levels were greater in fibroblasts and patient-derived iPSCs than in the corresponding control cells. Patient-derived iPSCs expressed lower basal levels than control iPSCs of the genes encoding the Hh ligands Indian Hedgehog (IHH) and SHH, the Hh acetyltransferase HHAT, Wnt proteins, BMP4, and BMP6. Most of these genes were upregulated in patient-derived iPSCs grown in osteoblast differentiation medium (OBM) and downregulated in control iPSCs cultured in OBM. The expression of GLI1 and GLI2 substantially decreased in both control and patient-derived iPSCs cultured in OBM, whereas GLI3, SHH, and IHH were upregulated in patient-derived iPSCs and downregulated in control iPSCs grown in OBM. Activation of Smoothened by SAG in cells grown in OBM significantly enhanced alkaline phosphatase activity in patient-derived iPSCs compared with control iPSC lines. In summary, patient-derived iPSCs expressed lower basal levels than the control iPSCs of the genes encoding Hh, Wnt, and bone morphogenetic proteins, but their expression of these genes strongly increased under osteogenic conditions. These findings indicate that patient-derived iPSCs are hypersensitive to osteogenic induction. We propose that Hh signaling is constituently active in iPSCs from Gorlin syndrome patients, enhancing their response to osteogenic induction and contributing to disease-associated abnormalities. Public Library of Science 2017-10-31 /pmc/articles/PMC5663396/ /pubmed/29088246 http://dx.doi.org/10.1371/journal.pone.0186879 Text en © 2017 Hasegawa et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Hasegawa, Daigo
Ochiai-Shino, Hiromi
Onodera, Shoko
Nakamura, Takashi
Saito, Akiko
Onda, Takeshi
Watanabe, Katsuhito
Nishimura, Ken
Ohtaka, Manami
Nakanishi, Mahito
Kosaki, Kenjiro
Yamaguchi, Akira
Shibahara, Takahiko
Azuma, Toshifumi
Gorlin syndrome-derived induced pluripotent stem cells are hypersensitive to hedgehog-mediated osteogenic induction
title Gorlin syndrome-derived induced pluripotent stem cells are hypersensitive to hedgehog-mediated osteogenic induction
title_full Gorlin syndrome-derived induced pluripotent stem cells are hypersensitive to hedgehog-mediated osteogenic induction
title_fullStr Gorlin syndrome-derived induced pluripotent stem cells are hypersensitive to hedgehog-mediated osteogenic induction
title_full_unstemmed Gorlin syndrome-derived induced pluripotent stem cells are hypersensitive to hedgehog-mediated osteogenic induction
title_short Gorlin syndrome-derived induced pluripotent stem cells are hypersensitive to hedgehog-mediated osteogenic induction
title_sort gorlin syndrome-derived induced pluripotent stem cells are hypersensitive to hedgehog-mediated osteogenic induction
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5663396/
https://www.ncbi.nlm.nih.gov/pubmed/29088246
http://dx.doi.org/10.1371/journal.pone.0186879
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