Abstract

Work during the current funding cycle implicates NF-kappaB/Rel proteins in keratinocyte-intrinsic growth control. In studying this, we found that the RelA NF-kappaB subunit controls the levels of the positive cell cycle regulator, CDK4. RelA physically interacts with CDK4, lowering CDK4 levels in a proteasome inhibitor-sensitive manner to trigger growth arrest. Conversely, RelA -/-epidermis generated recently in our lab displays increased CDK4 levels and hyper-proliferation. In human keratinocytes, NF-kappaB blockade increases CDK4 to levels sufficient to facilitate Ras-driven neoplasia. Using Cdk4-/- mice, we determined that epidermal hyperproliferation induced by loss of NF-kappaB function is CDK4-dependent. This increased proliferation is also dependent on the NF-kappaB-activating receptor, TNFR1, as shown by generating RelA-/-Tnfrl-/-epidermis. TNFR1 activates other signaling pathways besides IKK/NF-kappaB, notably the JNK cascade. In cells and tissue, NF-kappaB inhibition leads to JNK activation and JNK inhibitors block the hyper-proliferation that characterizes RelA -/- keratinocytes. In addition, RelA inhibits JNK activation, suggesting that epidermal RelA may oppose pro-proliferative signals from TNFR1 and JNK. Moreover, the majority of spontaneous human SCCs studied display evidence of simultaneous NF-kappaB blockade and JNK activation. These findings lead us to propose a model in which NF-kappaB RelA regulates epidermal proliferation in a manner involving the suppression of CDK4 protein levels and the opposition of the growth promoting action of TNFR1-JNK. First, we plan to define the mechanisms mediating CDK4 down regulation by NF-kappaB RelA in epidermal cells. To do this, we will define the nature and importance of the physical interactions between RelA and CDK4 as well as their impact on proteins involved in CDK4 stabilization and function. Second, we plan to characterize additional mechanisms involved in the increased epidermal proliferation induced by NF-kappaB inhibition. We will define the effects of altering the balance between JNK and NF-kappaB pathway function on epidermal homeostasis and neoplasia. Furthermore, we will define the contributions of TNFR1 to human epidermal neoplasia driven by NF-kappaB blockade. Over the proposed funding period, we plan to further define the mechanisms through which NFkappaB regulates growth of both normal and neoplastic epidermal tissue.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR045192-09
Application #
7173024
Study Section
Special Emphasis Panel (ZRG1-GMA-1 (01))
Program Officer
Baker, Carl
Project Start
1999-02-27
Project End
2009-01-31
Budget Start
2007-02-01
Budget End
2008-01-31
Support Year
9
Fiscal Year
2007
Total Cost
$343,961
Indirect Cost

  Institution

Name
Stanford University
Department
Dermatology
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Pattison, Jillian M; Melo, Sandra P; Piekos, Samantha N et al. (2018) Retinoic acid and BMP4 cooperate with p63 to alter chromatin dynamics during surface epithelial commitment. Nat Genet 50:1658-1665
Bao, Xiaomin; Siprashvili, Zurab; Zarnegar, Brian J et al. (2017) CSNK1a1 Regulates PRMT1 to Maintain the Progenitor State in Self-Renewing Somatic Tissue. Dev Cell 43:227-239.e5
Rubin, Adam J; Barajas, Brook C; Furlan-Magaril, Mayra et al. (2017) Lineage-specific dynamic and pre-established enhancer-promoter contacts cooperate in terminal differentiation. Nat Genet 49:1522-1528
Lopez-Pajares, Vanessa; Qu, Kun; Zhang, Jiajing et al. (2015) A LncRNA-MAF:MAFB transcription factor network regulates epidermal differentiation. Dev Cell 32:693-706
Bao, Xiaomin; Rubin, Adam J; Qu, Kun et al. (2015) A novel ATAC-seq approach reveals lineage-specific reinforcement of the open chromatin landscape via cooperation between BAF and p63. Genome Biol 16:284
Bhaduri, Aparna; Ungewickell, Alexander; Boxer, Lisa D et al. (2015) Network Analysis Identifies Mitochondrial Regulation of Epidermal Differentiation by MPZL3 and FDXR. Dev Cell 35:444-57
Sun, Bryan K; Boxer, Lisa D; Ransohoff, Julia D et al. (2015) CALML5 is a ZNF750- and TINCR-induced protein that binds stratifin to regulate epidermal differentiation. Genes Dev 29:2225-30
Sun, Bryan K; Siprashvili, Zurab; Khavari, Paul A (2014) Advances in skin grafting and treatment of cutaneous wounds. Science 346:941-5
Boxer, Lisa D; Barajas, Brook; Tao, Shiying et al. (2014) ZNF750 interacts with KLF4 and RCOR1, KDM1A, and CTBP1/2 chromatin regulators to repress epidermal progenitor genes and induce differentiation genes. Genes Dev 28:2013-26
Lopez-Pajares, Vanessa; Yan, Karen; Zarnegar, Brian J et al. (2013) Genetic pathways in disorders of epidermal differentiation. Trends Genet 29:31-40

Showing the most recent 10 out of 31 publications