Targeting neurotrophin and nitric oxide signaling to treat spinal cord injury and associated neurogenic bladder overactivity

Youko Ikeda; Irina Zabbarova; Pradeep Tyagi; T Kevin Hitchens; Amanda Wolf-Johnston; Peter Wipf; Anthony Kanai

doi:10.1016/j.cont.2022.100014

Targeting neurotrophin and nitric oxide signaling to treat spinal cord injury and associated neurogenic bladder overactivity

Continence (Amst). 2022 Mar:1:100014. doi: 10.1016/j.cont.2022.100014. Epub 2022 Mar 18.

Authors

Youko Ikeda^{1

2}, Irina Zabbarova¹, Pradeep Tyagi³, T Kevin Hitchens⁴, Amanda Wolf-Johnston¹, Peter Wipf⁵, Anthony Kanai^{1

2}

Affiliations

¹ University of Pittsburgh, School of Medicine, Department of Medicine, Renal-Electrolyte Division, USA.
² University of Pittsburgh, School of Medicine, Department of Pharmacology & Chemical Biology, USA.
³ University of Pittsburgh, School of Medicine, Department of Urology, USA.
⁴ University of Pittsburgh, School of Medicine, Animal Imaging Center, USA.
⁵ University of Pittsburgh, Dietrich School of Arts and Sciences, Department of Chemistry, USA.

Abstract

Purpose or the research: Nearly 300,000 people are affected by spinal cord injury (SCI) with approximately 18,000 new cases annually, according to the National SCI Statistics Center. SCI affects physical mobility and impairs the function of multiple internal organs to cause lower urinary tract (LUT) dysfunctions manifesting as detrusor sphincter dyssynergia (DSD) and neurogenic detrusor overactivity (NDO) with detrimental consequences to the quality of life and increased morbidity. Multiple lines of evidence now support time dependent evolution of the complex SCI pathology which requires a multipronged treatment approach of immediate, specialized care after spinal cord trauma bookended by physical rehabilitation to improve the clinical outcomes. Instead of one size fits all treatment approach, we propose adaptive drug treatment to counter the time dependent evolution of SCI pathology, with three small molecule drugs with distinctive sites of action for the recovery of multiple functions.

Principal results: Our findings demonstrate the improvement in the recovery of hindlimb mobility and bladder function of spinal cord contused mice following administration of small molecules targeting neurotrophin receptors, LM11A-31 and LM22B-10. While LM11A-31 reduced the cell death in the spinal cord, LM22B-10 promoted cell survival and axonal growth. Moreover, the soluble guanylate cyclase (sGC) activator, cinaciguat, enhanced the revascularization of the SCI injury site to promote vessel formation, dilation, and increased perfusion.

Major conclusions: Our adaptive three drug cocktail targets different stages of SCI and LUTD pathology: neuroprotective effect of LM11A-31 retards the cell death that occurs in the early stages of SCI; and LM22B-10 and cinaciguat promote neural remodeling and reperfusion at later stages to repair spinal cord scarring, DSD and NDO. LM11A-31 and cinaciguat have passed phase I and IIa clinical trials and possess significant potential for accelerated clinical testing in SCI/LUTD patients.

Keywords: Detrusor sphincter dyssynergia (DSD); Neurogenic detrusor overactivity (NDO); Soluble guanylate cyclase (sGC) activators; Spinal cord injury/contusion (SCI/SCC); TrkB/C receptors; p75 neurotrophin receptor (p75NTR).

Grants and funding

R01 DK098361/DK/NIDDK NIH HHS/United States