Abstract

Glucocorticoids (or simply steroids) remain the primary therapy for treating asthma. The glucocorticoid receptor (GR) is a potent transcription factor that, in response to glucocorticoids, can bind to DNA and directly induce the expression of numerous downstream genes. However, a distinct mechanism in which GR tethers to and represses inflammatory transcription factors such as NFkB (i.e. ?transrepression?) has long been viewed as central to steroid efficacy in asthma. Despite this dogma, airway cell data directly supporting the transrepression model are limited, and there remains considerable uncertainty regarding the mechanistic underpinning of steroid activity in the asthmatic airway. This knowledge gap has hampered efforts to improve steroid-based therapies, which cause debilitating side effects when used systemically to treat severe asthma. In this proposal, we will test the innovative hypothesis that therapeutic effects of steroids in airway smooth muscle (ASM), which exhibits extensive remodeling and cytokine secretion in difficult-to-treat asthma, are mediated through GR-based gene induction. Supporting this notion, our preliminary data has defined a pathway in which GR induces the Kruppel-like transcription factor, KLF15, which we have shown is a potent repressor of ASM remodeling. Our data further suggest that GR and KLF15 cooperatively induce CDKN1C, which is a cell cycle inhibitor, and PLCD1, a cytoskeletal regulator that appears to block smooth muscle actin expression in ASM. Thus, our data implicate steroid-induced pathways and cooperation between GR and KLF15 as potentially repressing pathologic ASM remodeling. Moreover, our data indicate that steroid-mediated repression of ASM cytokine expression also involves GR-mediated gene induction, in this case through a surprising cooperative relationship between GR and the prototypical pro-inflammatory transcription factor, NFB. Indeed, entirely orthogonal to the transrepression model, our data suggest that GR cooperates with NF?B to induce the expression of key anti-inflammatory genes such as A20, which is a potent negative feedback regulator of TNF and TLR signaling whose dysfunction is implicated in promoting asthma pathogenesis. Thus, cooperation between GR and factors such as KLF15 and NFkB, leading to gene induction, appears to be a central mechanism of steroid activity in ASM. However, the mechanistic basis for induction of CDKN1C and PLCD1 by GR and KLF15 has yet to be defined, and the precise role of these targets in repressing or reversing asthmatic ASM remodeling remains to be elucidated, Similarly, although our data support a role for GR-NFkB cooperative regulation of A20 in repressing ASM cytokine secretion, the genome-wide extent of GR- NFkB cooperation in ASM, and the in vivo consequences of GR-NFkB cooperation are not known. Thus, the goals of this proposal are: (1) to determine the mechanistic basis and consequences of GR-KLF15 cooperative gene induction, with a specific focus on regulation and phenotypic effects of CDKN1C and PLCD1 in ASM remodeling; (2) to determine the role of cooperation between GR and NFkB in mediating cytokine repression in ASM, with a specific focus on GR-NFkB cooperative regulation of A20 and the ASM-specific role of A20 in vivo in murine models of allergic airway disease; and (3) determine whether ASM from asthma patients exhibits perturbations in these novel pathways controlled by GR-mediated gene induction. In addition, through studying freshly isolated ASM from donor lungs, we will provide important insights into correlations between fresh and cultured ASM, particularly with respect to steroid-mediated gene induction and resistance. Taken together, this proposal will provide detailed molecular insight into the mechanisms underpinning GR function in ASM. This has broad implications for developing novel asthma therapeutics that selectively target severe airway remodeling and refractory inflammation in severe asthma.

Public Health Relevance

PHR: In the United States, asthma afflicts over 20 million people and is associated with yearly health care expenditures of over 18 billion dollars. Importantly, a large share of these costs go to the treatment of poorly controlled asthma. By exploring the molecular pathways controlled by glucocorticoids, which are cost-effective asthma therapy in many patients, we will uncover new targets for better asthma treatment and expand our understanding of how airway inflammation and asthma-associated airway thickening can be controlled.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL109557-07
Application #
9525385
Study Section
Lung Cellular, Molecular, and Immunobiology Study Section (LCMI)
Program Officer
Lachowicz-Scroggins, Marrah Elizabeth
Project Start
2012-04-15
Project End
2021-05-31
Budget Start
2018-06-01
Budget End
2019-05-31
Support Year
7
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
National Jewish Health
Department
Type
DUNS #
076443019
City
Denver
State
CO
Country
United States
Zip Code
80206

  Publications

Evans, Christopher M; Seibold, Max A; Gerber, Anthony N (2018) SPDEFending the Lung through Mucin Expression. Am J Respir Cell Mol Biol 59:287-288
Newton, Robert; Shah, Suharsh; Altonsy, Mohammed O et al. (2017) Glucocorticoid and cytokine crosstalk: Feedback, feedforward, and co-regulatory interactions determine repression or resistance. J Biol Chem 292:7163-7172
Sasse, Sarah K; Kadiyala, Vineela; Danhorn, Thomas et al. (2017) Glucocorticoid Receptor ChIP-Seq Identifies PLCD1 as a KLF15 Target that Represses Airway Smooth Muscle Hypertrophy. Am J Respir Cell Mol Biol 57:226-237
Altonsy, Mohammed O; Mostafa, Mahmoud M; Gerber, Anthony N et al. (2017) Long-acting ?2-agonists promote glucocorticoid-mediated repression of NF-?B by enhancing expression of the feedback regulator TNFAIP3. Am J Physiol Lung Cell Mol Physiol 312:L358-L370
Kraft, Monica; Gerber, Anthony N; Szefler, Stanley J et al. (2016) Introduction to the 58th Annual Thomas L. Petty Aspen Lung Conference: Asthma 2015: Mechanisms to Personalized Medicine. Ann Am Thorac Soc 13 Suppl 1:S23-4
Kadiyala, Vineela; Sasse, Sarah K; Altonsy, M Omar et al. (2016) Cistrome Analysis of Glucocorticoid Receptor Activity in Bronchial Epithelial Cells Defines Novel Mechanisms of Steroid Efficacy. Ann Am Thorac Soc 13 Suppl 1:S103
Sasse, Sarah K; Altonsy, Mohammed O; Kadiyala, Vineela et al. (2016) Glucocorticoid and TNF signaling converge at A20 (TNFAIP3) to repress airway smooth muscle cytokine expression. Am J Physiol Lung Cell Mol Physiol 311:L421-32
Kadiyala, Vineela; Sasse, Sarah K; Altonsy, Mohammed O et al. (2016) Cistrome-based Cooperation between Airway Epithelial Glucocorticoid Receptor and NF-?B Orchestrates Anti-inflammatory Effects. J Biol Chem 291:12673-87
Gerber, Anthony N (2015) Glucocorticoids and the Lung. Adv Exp Med Biol 872:279-98
Sasse, Sarah K; Zuo, Zheng; Kadiyala, Vineela et al. (2015) Response Element Composition Governs Correlations between Binding Site Affinity and Transcription in Glucocorticoid Receptor Feed-forward Loops. J Biol Chem 290:19756-69

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