m6A mRNA methylation facilitates resolution of naïve pluripotency toward differentiation

Shay Geula; Sharon Moshitch-Moshkovitz; Dan Dominissini; Abed Al Fatah Mansour; Nitzan Kol; Mali Salmon-Divon; Vera Hershkovitz; Eyal Peer; Nofar Mor; Yair S. Manor; Moshe Shay Ben-Haim; Eran Eyal; Sharon Yunger; Yishay Pinto; Diego Adhemar Jaitin; Sergey Viukov; Yoach Rais; Vladislav Krupalnik; Elad Chomsky; Mirie Zerbib; Itay Maza; Yoav Rechavi; Rada Massarwa; Suhair Hanna; Ido Amit; Erez Y. Levanon; Ninette Amariglio; Noam Stern-Ginossar; Noa Novershtern; Gideon Rechavi; Jacob H. Hanna

doi:10.1126/science.1261417

m⁶A mRNA methylation facilitates resolution of naïve pluripotency toward differentiation

Shay Geula, Sharon Moshitch-Moshkovitz, Dan Dominissini, Abed Al Fatah Mansour, Nitzan Kol, Mali Salmon-Divon, Vera Hershkovitz, Eyal Peer, Nofar Mor, Yair S. Manor, Moshe Shay Ben-Haim, Eran Eyal, Sharon Yunger, Yishay Pinto, Diego Adhemar Jaitin, Sergey Viukov, Yoach Rais, Vladislav Krupalnik, Elad Chomsky, Mirie ZerbibItay Maza, Yoav Rechavi, Rada Massarwa, Suhair Hanna, Ido Amit, Erez Y. Levanon, Ninette Amariglio, Noam Stern-Ginossar, Noa Novershtern, Gideon Rechavi, Jacob H. Hanna

نتاج البحث: نشر في مجلة › مقالة › مراجعة النظراء

1322 اقتباسات (Scopus)

ملخص

Naïve and primed pluripotent states retain distinct molecular properties, yet limited knowledge exists on how their state transitions are regulated. Here, we identify Mettl3, an N⁶-methyladenosine (m⁶A) transferase, as a regulator for terminating murine naïve pluripotency. Mettl3 knockout preimplantation epiblasts and naïve embryonic stem cells are depleted for m⁶A inmRNAs, yet are viable. However, they fail to adequately terminate their naïve state and, subsequently, undergo aberrant and restricted lineage priming at the postimplantation stage, which leads to early embryonic lethality. m⁶A predominantly and directly reduces mRNA stability, including that of key naïve pluripotency-promoting transcripts. This study highlights a critical role for an mRNA epigenetic modification in vivo and identifies regulatory modules that functionally influence naïve and primed pluripotency in an opposing manner.

اللغة الأصلية	الإنجليزيّة
الصفحات (من إلى)	1002-1006
عدد الصفحات	5
دورية	Science
مستوى الصوت	347
رقم الإصدار	6225
المعرِّفات الرقمية للأشياء	https://doi.org/10.1126/science.1261417
حالة النشر	نُشِر - 27 فبراير 2015
منشور خارجيًا	نعم

الوصول إلى المستند

10.1126/science.1261417

الملفات والروابط الأخرى

Link to publication in Scopus

قم بذكر هذا

Geula, S., Moshitch-Moshkovitz, S., Dominissini, D., Mansour, A. A. F., Kol, N., Salmon-Divon, M., Hershkovitz, V., Peer, E., Mor, N., Manor, Y. S., Ben-Haim, M. S., Eyal, E., Yunger, S., Pinto, Y., Jaitin, D. A., Viukov, S., Rais, Y., Krupalnik, V., Chomsky, E., ... Hanna, J. H. (2015). m⁶A mRNA methylation facilitates resolution of naïve pluripotency toward differentiation. Science, 347(6225), 1002-1006. https://doi.org/10.1126/science.1261417

@article{6fe1349f5f654468a778f8a449bb37fb,

title = "m6A mRNA methylation facilitates resolution of na{\"i}ve pluripotency toward differentiation",

abstract = "Na{\"i}ve and primed pluripotent states retain distinct molecular properties, yet limited knowledge exists on how their state transitions are regulated. Here, we identify Mettl3, an N6-methyladenosine (m6A) transferase, as a regulator for terminating murine na{\"i}ve pluripotency. Mettl3 knockout preimplantation epiblasts and na{\"i}ve embryonic stem cells are depleted for m6A inmRNAs, yet are viable. However, they fail to adequately terminate their na{\"i}ve state and, subsequently, undergo aberrant and restricted lineage priming at the postimplantation stage, which leads to early embryonic lethality. m6A predominantly and directly reduces mRNA stability, including that of key na{\"i}ve pluripotency-promoting transcripts. This study highlights a critical role for an mRNA epigenetic modification in vivo and identifies regulatory modules that functionally influence na{\"i}ve and primed pluripotency in an opposing manner.",

author = "Shay Geula and Sharon Moshitch-Moshkovitz and Dan Dominissini and Mansour, \{Abed Al Fatah\} and Nitzan Kol and Mali Salmon-Divon and Vera Hershkovitz and Eyal Peer and Nofar Mor and Manor, \{Yair S.\} and Ben-Haim, \{Moshe Shay\} and Eran Eyal and Sharon Yunger and Yishay Pinto and Jaitin, \{Diego Adhemar\} and Sergey Viukov and Yoach Rais and Vladislav Krupalnik and Elad Chomsky and Mirie Zerbib and Itay Maza and Yoav Rechavi and Rada Massarwa and Suhair Hanna and Ido Amit and Levanon, \{Erez Y.\} and Ninette Amariglio and Noam Stern-Ginossar and Noa Novershtern and Gideon Rechavi and Hanna, \{Jacob H.\}",

year = "2015",

month = feb,

day = "27",

doi = "10.1126/science.1261417",

language = "אנגלית",

volume = "347",

pages = "1002--1006",

journal = "Science",

issn = "0036-8075",

publisher = "American Association for the Advancement of Science",

number = "6225",

}

Geula, S, Moshitch-Moshkovitz, S, Dominissini, D, Mansour, AAF, Kol, N, Salmon-Divon, M, Hershkovitz, V, Peer, E, Mor, N, Manor, YS, Ben-Haim, MS, Eyal, E, Yunger, S, Pinto, Y, Jaitin, DA, Viukov, S, Rais, Y, Krupalnik, V, Chomsky, E, Zerbib, M, Maza, I, Rechavi, Y, Massarwa, R, Hanna, S, Amit, I, Levanon, EY, Amariglio, N, Stern-Ginossar, N, Novershtern, N, Rechavi, G & Hanna, JH 2015, 'm⁶A mRNA methylation facilitates resolution of naïve pluripotency toward differentiation', Science, المجلد 347, رقم 6225, الصفحات 1002-1006. https://doi.org/10.1126/science.1261417

TY - JOUR

T1 - m6A mRNA methylation facilitates resolution of naïve pluripotency toward differentiation

AU - Geula, Shay

AU - Moshitch-Moshkovitz, Sharon

AU - Dominissini, Dan

AU - Mansour, Abed Al Fatah

AU - Kol, Nitzan

AU - Salmon-Divon, Mali

AU - Hershkovitz, Vera

AU - Peer, Eyal

AU - Mor, Nofar

AU - Manor, Yair S.

AU - Ben-Haim, Moshe Shay

AU - Eyal, Eran

AU - Yunger, Sharon

AU - Pinto, Yishay

AU - Jaitin, Diego Adhemar

AU - Viukov, Sergey

AU - Rais, Yoach

AU - Krupalnik, Vladislav

AU - Chomsky, Elad

AU - Zerbib, Mirie

AU - Maza, Itay

AU - Rechavi, Yoav

AU - Massarwa, Rada

AU - Hanna, Suhair

AU - Amit, Ido

AU - Levanon, Erez Y.

AU - Amariglio, Ninette

AU - Stern-Ginossar, Noam

AU - Novershtern, Noa

AU - Rechavi, Gideon

AU - Hanna, Jacob H.

PY - 2015/2/27

Y1 - 2015/2/27

N2 - Naïve and primed pluripotent states retain distinct molecular properties, yet limited knowledge exists on how their state transitions are regulated. Here, we identify Mettl3, an N6-methyladenosine (m6A) transferase, as a regulator for terminating murine naïve pluripotency. Mettl3 knockout preimplantation epiblasts and naïve embryonic stem cells are depleted for m6A inmRNAs, yet are viable. However, they fail to adequately terminate their naïve state and, subsequently, undergo aberrant and restricted lineage priming at the postimplantation stage, which leads to early embryonic lethality. m6A predominantly and directly reduces mRNA stability, including that of key naïve pluripotency-promoting transcripts. This study highlights a critical role for an mRNA epigenetic modification in vivo and identifies regulatory modules that functionally influence naïve and primed pluripotency in an opposing manner.

AB - Naïve and primed pluripotent states retain distinct molecular properties, yet limited knowledge exists on how their state transitions are regulated. Here, we identify Mettl3, an N6-methyladenosine (m6A) transferase, as a regulator for terminating murine naïve pluripotency. Mettl3 knockout preimplantation epiblasts and naïve embryonic stem cells are depleted for m6A inmRNAs, yet are viable. However, they fail to adequately terminate their naïve state and, subsequently, undergo aberrant and restricted lineage priming at the postimplantation stage, which leads to early embryonic lethality. m6A predominantly and directly reduces mRNA stability, including that of key naïve pluripotency-promoting transcripts. This study highlights a critical role for an mRNA epigenetic modification in vivo and identifies regulatory modules that functionally influence naïve and primed pluripotency in an opposing manner.

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DO - 10.1126/science.1261417

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