Overexpressing TPTE2 (TPIP), a homolog of the human tumor suppressor gene PTEN, rescues the abnormal phenotype of the PTEN(−/−) mutant

One possible approach to normalize mutant cells that are metastatic and tumorigenic, is to upregulate a functionally similar homolog of the mutated gene. Here we have explored this hypothesis by generating an overexpressor of TPTE2 (TPIP), a homolog of PTEN, in PTEN(−/−) mutants, the latter generate...

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Autores principales: Lusche, Daniel F., Buchele, Emma C., Russell, Kanoe B., Soll, Benjamin A., Vitolo, Michele I., Klemme, Michael R., Wessels, Deborah J., Soll, David R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5940379/
https://www.ncbi.nlm.nih.gov/pubmed/29765523
http://dx.doi.org/10.18632/oncotarget.24941
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author Lusche, Daniel F.
Buchele, Emma C.
Russell, Kanoe B.
Soll, Benjamin A.
Vitolo, Michele I.
Klemme, Michael R.
Wessels, Deborah J.
Soll, David R.
author_facet Lusche, Daniel F.
Buchele, Emma C.
Russell, Kanoe B.
Soll, Benjamin A.
Vitolo, Michele I.
Klemme, Michael R.
Wessels, Deborah J.
Soll, David R.
author_sort Lusche, Daniel F.
collection PubMed
description One possible approach to normalize mutant cells that are metastatic and tumorigenic, is to upregulate a functionally similar homolog of the mutated gene. Here we have explored this hypothesis by generating an overexpressor of TPTE2 (TPIP), a homolog of PTEN, in PTEN(−/−) mutants, the latter generated by targeted mutagenesis of a human epithelial cell line. Overexpression of TPTE2 normalized phenotypic changes associated with the PTEN mutation. The PTEN(−/−)-associated changes rescued by overexpressing TPTE2 included 1) accelerated wound healing in the presence or absence of added growth factors (GFs), 2) increased division rates on a 2D substrate in the presence of GFs, 3) adhesion and viability on a 2D substrate in the absence of GFs, 4) viability in a 3D Matrigel model in the absence of GFs and substrate adhesion 5) loss of apoptosis-associated annexin V cell surface binding sites. The results justify further exploration into the possibility that upregulating TPTE2 by a drug may reverse metastatic and tumorigenic phenotypes mediated in part by a mutation in PTEN. This strategy may also be applicable to other tumorigenic mutations in which a homolog to the mutated gene is present and can substitute functionally.
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spelling pubmed-59403792018-05-15 Overexpressing TPTE2 (TPIP), a homolog of the human tumor suppressor gene PTEN, rescues the abnormal phenotype of the PTEN(−/−) mutant Lusche, Daniel F. Buchele, Emma C. Russell, Kanoe B. Soll, Benjamin A. Vitolo, Michele I. Klemme, Michael R. Wessels, Deborah J. Soll, David R. Oncotarget Research Paper One possible approach to normalize mutant cells that are metastatic and tumorigenic, is to upregulate a functionally similar homolog of the mutated gene. Here we have explored this hypothesis by generating an overexpressor of TPTE2 (TPIP), a homolog of PTEN, in PTEN(−/−) mutants, the latter generated by targeted mutagenesis of a human epithelial cell line. Overexpression of TPTE2 normalized phenotypic changes associated with the PTEN mutation. The PTEN(−/−)-associated changes rescued by overexpressing TPTE2 included 1) accelerated wound healing in the presence or absence of added growth factors (GFs), 2) increased division rates on a 2D substrate in the presence of GFs, 3) adhesion and viability on a 2D substrate in the absence of GFs, 4) viability in a 3D Matrigel model in the absence of GFs and substrate adhesion 5) loss of apoptosis-associated annexin V cell surface binding sites. The results justify further exploration into the possibility that upregulating TPTE2 by a drug may reverse metastatic and tumorigenic phenotypes mediated in part by a mutation in PTEN. This strategy may also be applicable to other tumorigenic mutations in which a homolog to the mutated gene is present and can substitute functionally. Impact Journals LLC 2018-04-20 /pmc/articles/PMC5940379/ /pubmed/29765523 http://dx.doi.org/10.18632/oncotarget.24941 Text en Copyright: © 2018 Lusche et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License 3.0 (http://creativecommons.org/licenses/by/3.0/) (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Lusche, Daniel F.
Buchele, Emma C.
Russell, Kanoe B.
Soll, Benjamin A.
Vitolo, Michele I.
Klemme, Michael R.
Wessels, Deborah J.
Soll, David R.
Overexpressing TPTE2 (TPIP), a homolog of the human tumor suppressor gene PTEN, rescues the abnormal phenotype of the PTEN(−/−) mutant
title Overexpressing TPTE2 (TPIP), a homolog of the human tumor suppressor gene PTEN, rescues the abnormal phenotype of the PTEN(−/−) mutant
title_full Overexpressing TPTE2 (TPIP), a homolog of the human tumor suppressor gene PTEN, rescues the abnormal phenotype of the PTEN(−/−) mutant
title_fullStr Overexpressing TPTE2 (TPIP), a homolog of the human tumor suppressor gene PTEN, rescues the abnormal phenotype of the PTEN(−/−) mutant
title_full_unstemmed Overexpressing TPTE2 (TPIP), a homolog of the human tumor suppressor gene PTEN, rescues the abnormal phenotype of the PTEN(−/−) mutant
title_short Overexpressing TPTE2 (TPIP), a homolog of the human tumor suppressor gene PTEN, rescues the abnormal phenotype of the PTEN(−/−) mutant
title_sort overexpressing tpte2 (tpip), a homolog of the human tumor suppressor gene pten, rescues the abnormal phenotype of the pten(−/−) mutant
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5940379/
https://www.ncbi.nlm.nih.gov/pubmed/29765523
http://dx.doi.org/10.18632/oncotarget.24941
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