Abstract

Actin is among the three highly conserved, highly abundant and highly important protein families in eukaryotic cells together with histones and tubulins. Actin can account for as much as 10% of total cellular proteins and is central in numerous functions in all eukaryotes involving motility, such as organelle movement, cell division, cell migration, cell shape maintenance, muscle contraction, nerve growth and many other functions critical to human health. However, the functions of actin in the cell nucleus have remained controversial for decades due to the lack of tractable systems to study nuclear actin. We have built a defined genetic and biochemical system in yeast to study the mysterious nuclear actin. This system allows us to define a distinct monomeric actin mechanism in the INO80 chromatin remodeling complex, which contrasts the established mechanism of cytoplasmic actin based on polymerization. Through continued study of the actin subunit in the INO80 complex, we have made a breakthrough discovery that actin undergoes a system of post-translational modification (PTMs) similar to histones. Given the numerous functions of actin in all eukaryotes, actin must be regulated to target distinct biological processes. The established paradigm that explains actin's participation in such a diverse range of functions is that actin can be directed to specific functions through interactions with actin- binding proteins (ABPs). Indeed, hundreds of ABPs involved in regulating actin biology have been identified. Our discovery of actin PTMs has led us to propose a new paradigm of actin regulation through actin PTMs. We hypothesize that distinct actin PTMs provide a major new mechanism for regulation of actin functions in biological processes, such as in transcription. Our initial study on actin R256 mono-methylation (R256me1) provides a validation of the actin PTM hypothesis, as R256me1 represents the first evolutionarily conserved mark for nuclear actin. Furthermore, actin R256me1 is implicated in transcription. Strikingly, mutations in the actin R256 residue (R258 in human) have been shown to cause human diseases, such as Thoracic Aortic Aneurysm and Dissection (TAAD), raising the possibility that actin PTMs contribute to TAAD through transcription. In the long term, we would like to establish the actin PTM hypothesis and discover its links to human diseases. In this proposal, we focus on the study of actin R256me1 in order to build the foundation for the actin PTM hypothesis. We propose to use genetic and biochemical approaches to define the enzymology of actin R256me1. Furthermore, we will investigate the biological roles of actin R256me1 in transcription and chromatin modification. Importantly, we will also determine the contribution of nuclear actin and actin PTMs to TAAD. The implications of the proposed studies are far reaching, as these pioneering actin PTM studies will open a new field in basic research and also provide a novel direction in medical research. Similar to the studies of histone PTMs, which exploded in the 1990s and revolutionized chromatin biology, we believe that the studies of nuclear actin and actin PTMs will usher in a new era in chromatin and actin biology.

Public Health Relevance

Actin is the most abundant protein in the cell and plays major roles in numerous processes in both cytoplasm and nucleus. We have discovered a wide range of modifications on nuclear actin. We will determine how nuclear actin modifications regulate genes and how defects in nuclear actin contribute to diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM093104-09
Application #
9669045
Study Section
Molecular Genetics A Study Section (MGA)
Program Officer
Xu, Jianhua
Project Start
2010-04-15
Project End
2021-03-31
Budget Start
2019-04-01
Budget End
2021-03-31
Support Year
9
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
University of Texas MD Anderson Cancer Center
Department
Internal Medicine/Medicine
Type
Overall Medical
DUNS #
800772139
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Shen, Jianfeng; Ju, Zhenlin; Zhao, Wei et al. (2018) ARID1A deficiency promotes mutability and potentiates therapeutic antitumor immunity unleashed by immune checkpoint blockade. Nat Med 24:556-562
Klages-Mundt, Naeh L; Kumar, Ashok; Zhang, Yuexuan et al. (2018) The Nature of Actin-Family Proteins in Chromatin-Modifying Complexes. Front Genet 9:398
Guo, Dong-Chuan; Duan, Xue-Yan; Regalado, Ellen S et al. (2017) Loss-of-Function Mutations in YY1AP1 Lead to Grange Syndrome and a Fibromuscular Dysplasia-Like Vascular Disease. Am J Hum Genet 100:21-30
Kapoor, Prabodh; Shen, Xuetong (2016) Stringing Nucleosome Necklaces in the Yeast Genome. Cell 167:600-601
Wang, Xuejuan; Chu, Huanyu; Lv, Mengjuan et al. (2016) Structure of the intact ATM/Tel1 kinase. Nat Commun 7:11655
Kapoor, Prabodh; Bao, Yunhe; Xiao, Jing et al. (2015) Phosphorylation-Dependent Enhancement of Rad53 Kinase Activity through the INO80 Chromatin Remodeling Complex. Mol Cell 58:863-9
Kapoor, Prabodh; Bao, Yunhe; Xiao, Jing et al. (2015) Regulation of Mec1 kinase activity by the SWI/SNF chromatin remodeling complex. Genes Dev 29:591-602
Kapoor, Prabodh; Shen, Xuetong (2014) Mechanisms of nuclear actin in chromatin-remodeling complexes. Trends Cell Biol 24:238-46
Kapoor, Prabodh; Chen, Mingming; Winkler, Duane David et al. (2013) Evidence for monomeric actin function in INO80 chromatin remodeling. Nat Struct Mol Biol 20:426-32
Falbo, Karina B; Shen, Xuetong (2012) Function of the INO80 chromatin remodeling complex in DNA replication. Front Biosci (Landmark Ed) 17:970-5

Showing the most recent 10 out of 12 publications