A deficiency screen of the 3rd chromosome for dominant modifiers of the Drosophila ER integral membrane protein, Jagunal

Author:

Ascencio Gerson1ORCID,de Cruz Matthew A1ORCID,Abuel Judy1ORCID,Alvarado Sydney1,Arriaga Yuma1,Conrad Emily1ORCID,Castro Alonso1ORCID,Eichelberger Katharine1ORCID,Galvan Laura1ORCID,Gundy Grace1ORCID,Garcia Jorge Alberto Inojoza1ORCID,Jimenez Alyssa1,Lu Nhien Tuyet1ORCID,Lugar Catharine1,Marania Ronald1ORCID,Mendsaikhan Tserendavaa1ORCID,Ortega Jose1ORCID,Nand Natasha1,Rodrigues Nicole S1ORCID,Shabazz Khayla1,Tam Cynnie1ORCID,Valenciano Emmanuel1ORCID,Hayzelden Clive1ORCID,Eritano Anthony S1ORCID,Riggs Blake1ORCID

Affiliation:

1. Department of Biology, San Francisco State University , 1600 Holloway Ave., San Francisco, CA 4132 , USA

Abstract

Abstract The mechanism surrounding chromosome inheritance during cell division has been well documented, however, organelle inheritance during mitosis is less understood. Recently, the endoplasmic reticulum (ER) has been shown to reorganize during mitosis, dividing asymmetrically in proneuronal cells prior to cell fate selection, indicating a programmed mechanism of inheritance. ER asymmetric partitioning in proneural cells relies on the highly conserved ER integral membrane protein, Jagunal (Jagn). Knockdown of Jagn in the compound Drosophila eye displays a pleotropic rough eye phenotype in 48% of the progeny. To identify genes involved in Jagn dependent ER partitioning pathway, we performed a dominant modifier screen of the 3rd chromosome for enhancers and suppressors of this Jagn-RNAi-induced rough eye phenotype. We screened through 181 deficiency lines covering the 3L and 3R chromosomes and identified 12 suppressors and 10 enhancers of the Jagn-RNAi phenotype. Based on the functions of the genes covered by the deficiencies, we identified genes that displayed a suppression or enhancement of the Jagn-RNAi phenotype. These include Division Abnormally Delayed (Dally), a heparan sulfate proteoglycan, the γ-secretase subunit Presenilin, and the ER resident protein Sec63. Based on our understanding of the function of these targets, there is a connection between Jagn and the Notch signaling pathway. Further studies will elucidate the role of Jagn and identified interactors within the mechanisms of ER partitioning during mitosis.

Funder

California State University Program for Education and Research in Biotechnology

National Science Foundation

Faculty Early Career Development Program

NSF Facilitating Research at Primary Undergraduate Institutions

NSF-MRI

NSF-EAR

NIH

NIH MS Bridges

NSF-STC, Center for Cellular Construction

Louis Stokes Alliance for Minority Participation

Genentech Foundation Scholars

Publisher

Oxford University Press (OUP)

Subject

Genetics (clinical),Genetics,Molecular Biology

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