Objective: To determine whether striatal CaV1.3 gene silencing ameliorates levodopa-induced dyskinesias (LID) in the preclinical gold-standard non-human primate (NHP) model without altering levodopa’s antiparkinsonian benefit.
Background: We previously reported that mRNA-level silencing of striatal CaV1.3 channels in young adult male parkinsonian rats prior to the introduction of levodopa could completely prevent LID induction even with prolonged dose escalation1. To advance our understanding of the potential clinical utility of this gene therapy approach, we are undertaking a second phase of investigations examining the ability of striatal CaV1.3 silencing to impact LID development in aged male and female parkinsonian macaques.
Method: Male and female Mauritian cynomolgous monkeys (23-24 yrs) received a unilateral intracarotid injection of the neurotoxin MPTP to induce unilateral parkinsonism. Two weeks later they began receiving intravenous MPTP injections (0.3-0.6 mg/kg) until significant bilateral parkinsonian motor signs appeared (~3mo). Cumulative stabilization of PD motor impairments occurred over ~8 mos (prolonged due to pandemic) prior to bilateral putaminal injections of AAV-CaV1.3-shRNA designed against primate/macaque CaV1.3 (N=2 male; N=2 female), or AAV-Scr-shRNA (N=1 male). A second cohort of N=2 Scr-shRNA, N=1 CaV-shRNA is ongoing. Levodopa:carbidopa (25:100; p.o., b.i.d., M-Fr) was administered at escalating doses (20mg/kg for 3.5mo; 30mg/kg for 1mo; 40mg/kg for 1mo). PD disability (PDD) ‘ON’ & ‘OFF’ levodopa, hand-reach task and LID were evaluated at regular intervals.
Results: LID was first observed post-vector (PV) wk16 on day 43 of 20mg/kg (peak dose LID severity scores: Scr=12.0; CaV=1.0+0.35, mean+SEM). LID severity continued to escalate in the Scr-shRNA subject but remained equally negligible in all CaV-shRNA subjects (peak LID severity, final day of 40mg/kg: Scr=29.0; CaV=2.8+0.65). This anti-dyskinogenic effect occurred in the presence of levodopa-induced rotations and decrease in cumulative PDD (Wks7-28 PV) ‘ON’ & ‘OFF’ levodopa (p<0.01-0.001, Freidman’s test & Dunn’s post-hoc).
Conclusion: Decreasing striatal expression of CaV1.3 in aged male & female NHPs can provide near complete protection against LID induction when gene therapy is administered to NHP with long-standing severe parkinsonian disability and prior to introduction of levodopa.
References: [1] Steece-Collier K, Stancati JA, Collier NJ, Sandoval IM, Mercado NM, Sortwell CE, Collier TJ, Manfredsson FP. Genetic silencing of striatal CaV1.3 prevents and ameliorates levodopa dyskinesia. Mov Disord. (2019) 34(5):697-707. PMID: 31002755
To cite this abstract in AMA style:
K. Steece-Collier, F. Manfredsson, S. Muller, M. Caulfield, M. Vander Werp, J. Stancati, Y. Chu, I. Sandoval, T. Collier, J. Kordower. Antidyskinetic Effects of CaV1.3 Calcium Channel Gene Silencing in Aged Male and Female Parkinsonian Macaques [abstract]. Mov Disord. 2022; 37 (suppl 2). https://www.mdsabstracts.org/abstract/antidyskinetic-effects-of-cav1-3-calcium-channel-gene-silencing-in-aged-male-and-female-parkinsonian-macaques/. Accessed November 21, 2024.« Back to 2022 International Congress
MDS Abstracts - https://www.mdsabstracts.org/abstract/antidyskinetic-effects-of-cav1-3-calcium-channel-gene-silencing-in-aged-male-and-female-parkinsonian-macaques/