Project Summary
Design of neuromodulatory devices targeting the kidney requires detailed knowledge of the structural
and functional neurobiology of renal nerves. Our current understanding is fairly rudimentary and based on
classical but outdated methodologies. For example, it is generally agreed that renal efferent nerves increase
renin release, stimulate sodium reabsorption, and decrease GFR secondary to arteriolar constriction. However,
the dose-response relationships for these effects are based on supramaximal electrical stimulation of renal
nerves in anesthetized animals. Recent studies in conscious animals suggest this dogma may be incorrect.
Even less is known regarding the structural and functional neurobiology of renal afferent nerves. Although it is
well accepted that the renal pelvic wall in densely innervated, preliminary findings in our laboratory, as well as
reports by others, suggest sensory nerves may also innervate vascular and tubular targets throughout the
kidney. However, the physiological role of renal afferent nerves is unclear. Finally, it is well established that the
afferent and efferent innervation of the kidney is heterogeneous. Distinct subsets of sympathetic renal nerves
express the neuropeptides NPY and VIP. In the afferent renal innervation there is partial overlap of expression
of the neuropeptides CGRP and SP and the capsaicin receptor TRPV1. In addition, our preliminary results
demonstrate for the first time the presence of renal afferent nerves that express the sensory neuron-specific
voltage-gated Na+ channel NaV1.8. The functional significance of the neurochemical diversity of renal afferent
and efferent nerves represents a critical gap in our understanding of neural control of kidney function.
Our central hypothesis is that efferent and afferent nerves with distinct neurochemical signatures
differentially control renal functions through their association with distinct renal structures. We will use state-of-
the-art neurophysiological and neuroanatomical approaches to generate an integrated functional and structural
map of neural control in the mouse kidney. We will also initiate translation of these finding to the human kidney
through comprehensive neuroanatomical analysis. In Specific Aim 1 will test the hypothesis that
neurochemically distinct renal nerves differentially control renal function. In Specific Aim 2 we will test the
hypothesis that neurochemically distinct renal nerves are associated with distinct structures in the
kidney. Finally, in Specific Aim 3 we will define the structural neurobiology of renal efferent and afferent
nerves, and their relationship to vascular, tubular and renal pelvis anatomy in the human kidney.
Public Health Relevance Statement
Project Narrative
The kidneys play an important role in the maintenance of body fluid homeostasis and cardiovascular function.
The proposed research will aid in the development of new device based therapies that target nerves that
control the kidney by increasing our understanding of the their anatomy and physiology.
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