Multiple congenital malformations arise from somatic mosaicism for constitutively active Pik3ca signaling

Recurrent missense mutations of the PIK3CA oncogene are among the most frequent drivers of human cancers. These often lead to constitutive activation of its product p110α, a phosphatidylinositol 3-kinase (PI3K) catalytic subunit. In addition to causing a broad range of cancers, the H1047R mutation i...

Descripción completa

Detalles Bibliográficos
Autores principales: Marechal, Elise, Poliard, Anne, Henry, Kilian, Moreno, Mathias, Legrix, Mathilde, Macagno, Nicolas, Mondielli, Grégoire, Fauquier, Teddy, Barlier, Anne, Etchevers, Heather C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Cell and Developmental Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9637999/
https://www.ncbi.nlm.nih.gov/pubmed/36353506
http://dx.doi.org/10.3389/fcell.2022.1013001
_version_ 1784825308621307904
author Marechal, Elise
Poliard, Anne
Henry, Kilian
Moreno, Mathias
Legrix, Mathilde
Macagno, Nicolas
Mondielli, Grégoire
Fauquier, Teddy
Barlier, Anne
Etchevers, Heather C.
author_facet Marechal, Elise
Poliard, Anne
Henry, Kilian
Moreno, Mathias
Legrix, Mathilde
Macagno, Nicolas
Mondielli, Grégoire
Fauquier, Teddy
Barlier, Anne
Etchevers, Heather C.
author_sort Marechal, Elise
collection PubMed
description Recurrent missense mutations of the PIK3CA oncogene are among the most frequent drivers of human cancers. These often lead to constitutive activation of its product p110α, a phosphatidylinositol 3-kinase (PI3K) catalytic subunit. In addition to causing a broad range of cancers, the H1047R mutation is also found in affected tissues of a distinct set of congenital tumors and malformations. Collectively termed PIK3CA-related disorders (PRDs), these lead to overgrowth of brain, adipose, connective and musculoskeletal tissues and/or blood and lymphatic vessel components. Vascular malformations are frequently observed in PRD, due to cell-autonomous activation of PI3K signaling within endothelial cells. These, like most muscle, connective tissue and bone, are derived from the embryonic mesoderm. However, important organ systems affected in PRDs are neuroectodermal derivatives. To further examine their development, we drove the most common post-zygotic activating mutation of Pik3ca in neural crest and related embryonic lineages. Outcomes included macrocephaly, cleft secondary palate and more subtle skull anomalies. Surprisingly, Pik3ca-mutant subpopulations of neural crest origin were also associated with widespread cephalic vascular anomalies. Mesectodermal neural crest is a major source of non-endothelial connective tissue in the head, but not the body. To examine the response of vascular connective tissues of the body to constitutive Pik3ca activity during development, we expressed the mutation by way of an Egr2 (Krox20) Cre driver. Lineage tracing led us to observe new lineages that had normally once expressed Krox20 and that may be co-opted in pathogenesis, including vascular pericytes and perimysial fibroblasts. Finally, Schwann cell precursors having transcribed either Krox20 or Sox10 and induced to express constitutively active PI3K were associated with vascular and other tumors. These murine phenotypes may aid discovery of new candidate human PRDs affecting craniofacial and vascular smooth muscle development as well as the reciprocal paracrine signaling mechanisms leading to tissue overgrowth.
format Online
Article
Text
id pubmed-9637999
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-96379992022-11-08 Multiple congenital malformations arise from somatic mosaicism for constitutively active Pik3ca signaling Marechal, Elise Poliard, Anne Henry, Kilian Moreno, Mathias Legrix, Mathilde Macagno, Nicolas Mondielli, Grégoire Fauquier, Teddy Barlier, Anne Etchevers, Heather C. Front Cell Dev Biol Cell and Developmental Biology Recurrent missense mutations of the PIK3CA oncogene are among the most frequent drivers of human cancers. These often lead to constitutive activation of its product p110α, a phosphatidylinositol 3-kinase (PI3K) catalytic subunit. In addition to causing a broad range of cancers, the H1047R mutation is also found in affected tissues of a distinct set of congenital tumors and malformations. Collectively termed PIK3CA-related disorders (PRDs), these lead to overgrowth of brain, adipose, connective and musculoskeletal tissues and/or blood and lymphatic vessel components. Vascular malformations are frequently observed in PRD, due to cell-autonomous activation of PI3K signaling within endothelial cells. These, like most muscle, connective tissue and bone, are derived from the embryonic mesoderm. However, important organ systems affected in PRDs are neuroectodermal derivatives. To further examine their development, we drove the most common post-zygotic activating mutation of Pik3ca in neural crest and related embryonic lineages. Outcomes included macrocephaly, cleft secondary palate and more subtle skull anomalies. Surprisingly, Pik3ca-mutant subpopulations of neural crest origin were also associated with widespread cephalic vascular anomalies. Mesectodermal neural crest is a major source of non-endothelial connective tissue in the head, but not the body. To examine the response of vascular connective tissues of the body to constitutive Pik3ca activity during development, we expressed the mutation by way of an Egr2 (Krox20) Cre driver. Lineage tracing led us to observe new lineages that had normally once expressed Krox20 and that may be co-opted in pathogenesis, including vascular pericytes and perimysial fibroblasts. Finally, Schwann cell precursors having transcribed either Krox20 or Sox10 and induced to express constitutively active PI3K were associated with vascular and other tumors. These murine phenotypes may aid discovery of new candidate human PRDs affecting craniofacial and vascular smooth muscle development as well as the reciprocal paracrine signaling mechanisms leading to tissue overgrowth. Frontiers Media S.A. 2022-10-24 /pmc/articles/PMC9637999/ /pubmed/36353506 http://dx.doi.org/10.3389/fcell.2022.1013001 Text en Copyright © 2022 Marechal, Poliard, Henry, Moreno, Legrix, Macagno, Mondielli, Fauquier, Barlier and Etchevers. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cell and Developmental Biology
Marechal, Elise
Poliard, Anne
Henry, Kilian
Moreno, Mathias
Legrix, Mathilde
Macagno, Nicolas
Mondielli, Grégoire
Fauquier, Teddy
Barlier, Anne
Etchevers, Heather C.
Multiple congenital malformations arise from somatic mosaicism for constitutively active Pik3ca signaling
title Multiple congenital malformations arise from somatic mosaicism for constitutively active Pik3ca signaling
title_full Multiple congenital malformations arise from somatic mosaicism for constitutively active Pik3ca signaling
title_fullStr Multiple congenital malformations arise from somatic mosaicism for constitutively active Pik3ca signaling
title_full_unstemmed Multiple congenital malformations arise from somatic mosaicism for constitutively active Pik3ca signaling
title_short Multiple congenital malformations arise from somatic mosaicism for constitutively active Pik3ca signaling
title_sort multiple congenital malformations arise from somatic mosaicism for constitutively active pik3ca signaling
topic Cell and Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9637999/
https://www.ncbi.nlm.nih.gov/pubmed/36353506
http://dx.doi.org/10.3389/fcell.2022.1013001
work_keys_str_mv AT marechalelise multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling
AT poliardanne multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling
AT henrykilian multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling
AT morenomathias multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling
AT legrixmathilde multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling
AT macagnonicolas multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling
AT mondielligregoire multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling
AT fauquierteddy multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling
AT barlieranne multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling
AT etcheversheatherc multiplecongenitalmalformationsarisefromsomaticmosaicismforconstitutivelyactivepik3casignaling

Ejemplares similares