Zac1 Is an Essential Transcription Factor for Cardiac Morphogenesis

Author:

Yuasa Shinsuke1,Onizuka Takeshi1,Shimoji Kenichiro1,Ohno Yohei1,Kageyama Toshimi1,Yoon Sung Han1,Egashira Toru1,Seki Tomohisa1,Hashimoto Hisayuki1,Nishiyama Takahiko1,Kaneda Ruri1,Murata Mitsushige1,Hattori Fumiyuki1,Makino Shinji1,Sano Motoaki1,Ogawa Satoshi1,Prall Owen W.J.1,Harvey Richard P.1,Fukuda Keiichi1

Affiliation:

1. From the Department of Regenerative Medicine and Advanced Cardiac Therapeutics (S.Y., T.O., K.S., Y.O., T.K., S.H.Y., T.E., T.S., H.H., T.N., R.K., M.M., F.H., S.M., M.S., K.F.); Cardiology Division (S.Y., T.O., K.S., Y.O., T.K., S.H.Y., T.E., T.S., H.H., T.N., M.M., S.O.), Department of Internal Medicine; and Center for Integrated Medical Research (S.Y., S.M.), Keio University School of Medicine, Tokyo, Japan; Victor Chang Cardiac Research Institute (O.W.J.P., R.P.H.), Darlinghurst, New South Wales...

Abstract

Rationale : The transcriptional networks guiding heart development remain poorly understood, despite the identification of several essential cardiac transcription factors. Objective : To isolate novel cardiac transcription factors, we performed gene chip analysis and found that Zac1 , a zinc finger-type transcription factor, was strongly expressed in the developing heart. This study was designed to investigate the molecular and functional role of Zac1 as a cardiac transcription factor. Methods and Results : Zac1 was strongly expressed in the heart from cardiac crescent stages and in the looping heart showed a chamber-restricted pattern. Zac1 stimulated luciferase reporter constructs driven by ANF, BNP , or α MHC promoters. Strong functional synergy was seen between Zac1 and Nkx2-5 on the ANF promoter, which carries adjacent Zac1 and Nkx2-5 DNA-binding sites. Zac1 directly associated with the ANF promoter in vitro and in vivo, and Zac1 and Nkx2-5 physically associated through zinc fingers 5 and 6 in Zac1, and the homeodomain in Nkx2-5. Zac1 is a maternally imprinted gene and is the first such gene found to be involved in heart development. Homozygous and paternally derived heterozygous mice carrying an interruption in the Zac1 locus showed decreased levels of chamber and myofilament genes, increased apoptotic cells, partially penetrant lethality and morphological defects including atrial and ventricular septal defects, and thin ventricular walls. Conclusions : Zac1 plays an essential role in the cardiac gene regulatory network. Our data provide a potential mechanistic link between Zac1 in cardiogenesis and congenital heart disease manifestations associated with genetic or epigenetic defects in an imprinted gene network.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine,Physiology

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