Abstract

Regulated intracellular proteolysis controls virtually every aspect of cell physiology. The process is highly selective, with individual protein half-live ranging from minutes to weeks. This selectivity is ensured by specific interactions between substrates and E3 ubiquitin ligase complexes, which mark proteins for degradation with a chain of ubiquitin moieties. Many E3 ligases are modular, based on a core scaffold, with interchangeable substrate-targeting subunits, which enables one piece of core machinery to ubiquitylate many different substrates. The cullin-RING ligase (CRL) family of complexes are the archetypes for these modular ubiquitin ligases, and CRL1 ligases, better known as the SKP1-CUL1-F-box protein (SCF) complexes, are the best characterized. SCFs use a family of F-box proteins (69 in humans) as substrate adaptors to mediate the ubiquitylation and consequent degradation of a large number of regulatory proteins involved in diverse processes. During the initial years of GM57587, my laboratory investigated how two SCF complexes (SCF- SKP2 and SCF-TrCP) and APC/C (a CRL-like ubiquitin ligase) target various regulators of cyclin dependent kinases (CDKs) for degradation. Subsequently, to broaden our knowledge of these remarkable enzymes, we asked whether any other members of the F-box protein family play important roles in controlling the cell division cycle. For example, during the last funding cycle, we found that cyclin F (FBXO1) controls genome integrity by coordinating production of deoxyribonucleotides with DNA replication; FBH1 (FBXO18) promotes DNA double strand breakage and apoptosis in response to DNA replication stress; and FBXO11 regulates cell quiescence and differentiation. We now propose a project exploring the integration of CRL- controlled cell cycle networks with DNA replication and the DNA damage response. Via proteomic techniques, we have identified putative CRL substrates involved in these processes, and using an interdisciplinary approach that incorporates biochemistry, molecular cell biology, and somatic cell genetics, we will characterize the molecular mechanisms and biological significance of the degradation of these novel substrates.

Public Health Relevance

Through the regulated proteolysis of a plethora of diverse substrates, cullin-RING ligases (CRLs) control a large number of processes at the cellular and organismal levels. The misregulated degradation of tumor suppressors or oncoproteins can drive tumorigenesis. Accordingly, CRLs can function as oncoproteins when overexpressed (if their substrates are tumor suppressors) or as tumor suppressors (if their substrates are oncoproteins). The clinical success of thalidomide and lenalidomide, two CRL ligase inhibitors used in the therapy of multiple myeloma, suggests the potential to develop drugs targeting other CRL ligases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM057587-18
Application #
9127963
Study Section
Cellular Signaling and Regulatory Systems Study Section (CSRS)
Program Officer
Melillo, Amanda A
Project Start
1998-04-03
Project End
2019-08-31
Budget Start
2016-09-01
Budget End
2017-08-31
Support Year
18
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
New York University
Department
Pathology
Type
Schools of Medicine
DUNS #
121911077
City
New York
State
NY
Country
United States
Zip Code
10016

  Publications

Galluzzi, Lorenzo; Vitale, Ilio; Aaronson, Stuart A et al. (2018) Molecular mechanisms of cell death: recommendations of the Nomenclature Committee on Cell Death 2018. Cell Death Differ 25:486-541
Kuchay, Shafi; Saeed, Mohsan; Giorgi, Carlotta et al. (2018) NS5A Promotes Constitutive Degradation of IP3R3 to Counteract Apoptosis Induced by Hepatitis C Virus. Cell Rep 25:833-840.e3
Rona, Gergely; Roberti, Domenico; Yin, Yandong et al. (2018) PARP1-dependent recruitment of the FBXL10-RNF68-RNF2 ubiquitin ligase to sites of DNA damage controls H2A.Z loading. Elife 7:
Mavrommati, Ioanna; Faedda, Roberta; Galasso, Giovanni et al. (2018) ?-TrCP- and Casein Kinase II-Mediated Degradation of Cyclin F Controls Timely Mitotic Progression. Cell Rep 24:3404-3412
Pae, Juhee; Cinalli, Ryan M; Marzio, Antonio et al. (2017) GCL and CUL3 Control the Switch between Cell Lineages by Mediating Localized Degradation of an RTK. Dev Cell 42:130-142.e7
Fehrenbacher, Nicole; Tojal da Silva, Israel; Ramirez, Craig et al. (2017) The G protein-coupled receptor GPR31 promotes membrane association of KRAS. J Cell Biol 216:2329-2338
Donato, Valerio; Bonora, Massimo; Simoneschi, Daniele et al. (2017) The TDH-GCN5L1-Fbxo15-KBP axis limits mitochondrial biogenesis in mouse embryonic stem cells. Nat Cell Biol 19:341-351
Kuchay, Shafi; Giorgi, Carlotta; Simoneschi, Daniele et al. (2017) PTEN counteracts FBXL2 to promote IP3R3- and Ca2+-mediated apoptosis limiting tumour growth. Nature 546:554-558
D'Alessandro, Matthew; Beesley, Stephen; Kim, Jae Kyoung et al. (2017) Stability of Wake-Sleep Cycles Requires Robust Degradation of the PERIOD Protein. Curr Biol 27:3454-3467.e8
Dankert, John F; Pagan, Julia K; Starostina, Natalia G et al. (2017) FEM1 proteins are ancient regulators of SLBP degradation. Cell Cycle 16:556-564

Showing the most recent 10 out of 112 publications