Abstract

Inappropriate activation of the renin angiotensin system (RAS) makes a critical contribution to the progression of chronic kidney disease (CKD). However, the effects of the RAS effector angiotensin (Ang) II on renal damage are tissue-specific. Stimulating type 1 angiotensin (AT1) receptors in the kidney drives blood pressure elevation and renal injury. By contrast, we have recently established that activating AT1 receptors directly on T lymphocytes suppresses pro-inflammatory Th1 cytokines and protects the kidney. Like angiotensin (Ang II), the transcription factor Twist1 acts in kidney cells to driv renal fibrosis but in immune cells to suppress NF-?b-dependent cytokine induction. To explain these analogous actions of Ang II and Twist1, we have discovered that Ang II induces Twist1 expression in macrophages and T lymphocytes. Nevertheless, in our new preliminary studies, Twist1 in T cells promotes blood pressure elevation and albuminuria in the Ang II-dependent hypertension model. This finding is completely unexpected based on the published literature that emphasizes cytokine suppression by Twist1 in T cells. Resolving this paradox, NF- ?B activation also drives transcription of TGF-? 9, a key effector cytokine of CD4+CD25+ T regulatory cells whose adoptive transfer can blunt the hypertensive response. We find that Twist1 in T cells limits the emergence of these CD4+CD25+ T cells following NF-?B stimulation. We therefore hypothesize that Twist1 in T cells promotes hypertension and renal injury during RAS activation by suppressing T regulatory cell functions. To test this hypothesis, we will subject mice lacking Twist1 solely in T cells to models of RAS- dependent hypertension and kidney damage. Whereas TGF-? in T lymphocytes mediates T regulatory cell functions, TGF-? in macrophages drives kidney fibrosis during RAS activation. Consistent with this notion, in our preliminary studies, Twist1-deficiency in macrophages permits exaggerated TGF-? and TNF-? expression, leading to augmented RAS-dependent kidney damage and fibrosis. However, we now find that these same cytokines can induce several Wnt ligand isoforms in kidney epithelial cells and that blocking Porcupine (PORC)-dependent secretion of these Wnts dramatically attenuates the extent of kidney damage and fibrosis. Thus, we posit that Twist1 in macrophages protects the kidney from injury and fibrosis by limiting cytokine-dependent Wnt generation in kidney epithelial cells. We will test this possibility using unpublished models of macrophage-specific Twist1 deficiency and kidney-specific PORC deficiency in conjunction with our kidney cross-transplantation strategy. Collectively, our studies will define for the first time the contribution of Twist1 in hematopoietic cell populations to blood pressure regulation and will discriminate novel mechanisms through which Twist1 modulates kidney damage and fibrosis. Given the importance of Twist1 not only to fibrosis but also to tumor metastasis, establishing these cell-specific actions of Twist1 in vivo will be critical to allow targeting of this pathway i patients with hypertension, tissue fibrosis, and cancer.

Public Health Relevance

Inappropriate activation of the renin angiotensin system (RAS) accelerates the progression of chronic kidney disease. This proposal explores how the transcription factor Twist1 modulates RAS-mediated renal damage by regulating a subset of T lymphocytes (Th1 cells). Understanding how Th1 immune responses influence angiotensin II-induced kidney injury should lead to more effective strategies for preventing progressive chronic kidney disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK087893-08
Application #
9443627
Study Section
Pathobiology of Kidney Disease Study Section (PBKD)
Program Officer
Abbott, Kevin C
Project Start
2010-08-01
Project End
2019-02-28
Budget Start
2018-03-01
Budget End
2019-02-28
Support Year
8
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Duke University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
044387793
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

Wen, Yi; Crowley, Steven D (2018) Renal effects of cytokines in hypertension. Curr Opin Nephrol Hypertens 27:70-76
Rucker, A Justin; Rudemiller, Nathan P; Crowley, Steven D (2018) Salt, Hypertension, and Immunity. Annu Rev Physiol 80:283-307
Rudemiller, Nathan P; Crowley, Steven D (2017) The role of chemokines in hypertension and consequent target organ damage. Pharmacol Res 119:404-411
Wu, Min; Zhang, Jian-Dong; Tang, Ri-Ning et al. (2017) Elevated PTH induces endothelial-to-chondrogenic transition in aortic endothelial cells. Am J Physiol Renal Physiol 312:F436-F444
Justin Rucker, A; Crowley, Steven D (2017) The role of macrophages in hypertension and its complications. Pflugers Arch 469:419-430
Rudemiller, Nathan P; Patel, Mehul B; Zhang, Jian-Dong et al. (2016) C-C Motif Chemokine 5 Attenuates Angiotensin II-Dependent Kidney Injury by Limiting Renal Macrophage Infiltration. Am J Pathol 186:2846-2856
Zhang, Jiandong; Rudemiller, Nathan P; Patel, Mehul B et al. (2016) Competing Actions of Type 1 Angiotensin II Receptors Expressed on T Lymphocytes and Kidney Epithelium during Cisplatin-Induced AKI. J Am Soc Nephrol 27:2257-64
Rudemiller, Nathan P; Crowley, Steven D (2016) Interactions Between the Immune and the Renin-Angiotensin Systems in Hypertension. Hypertension 68:289-96
Madan, Babita; Patel, Mehul B; Zhang, Jiandong et al. (2016) Experimental inhibition of porcupine-mediated Wnt O-acylation attenuates kidney fibrosis. Kidney Int 89:1062-1074
Zhang, Jiandong; Rudemiller, Nathan P; Patel, Mehul B et al. (2016) Interleukin-1 Receptor Activation Potentiates Salt Reabsorption in Angiotensin II-Induced Hypertension via the NKCC2 Co-transporter in the Nephron. Cell Metab 23:360-8

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