A Randomized, Crossover, Pharmacokinetic and Adhesion Performance Study of a Lidocaine Topical System 1.8% During Physical Activity and Heat Treatment in Healthy Subjects

Jeffrey Fudin; Erica L Wegrzyn; Emileigh Greuber; Kip Vought; Kalpana Patel; Sri Nalamachu

doi:10.2147/JPR.S238268

A Randomized, Crossover, Pharmacokinetic and Adhesion Performance Study of a Lidocaine Topical System 1.8% During Physical Activity and Heat Treatment in Healthy Subjects

J Pain Res. 2020 Jun 10:13:1359-1367. doi: 10.2147/JPR.S238268. eCollection 2020.

Authors

Jeffrey Fudin^{1

2

3

4}, Erica L Wegrzyn^{1

2

3}, Emileigh Greuber⁵, Kip Vought⁵, Kalpana Patel⁵, Sri Nalamachu⁶

Affiliations

¹ Samuel Stratton Department of Veterans Affairs Medical Center, Albany, NY, USA.
² Albany College of Pharmacy & Health Sciences, Albany, NY, USA.
³ Western New England University College of Pharmacy, Springfield, MA, USA.
⁴ Remitigate, LLC, Delmar, NY, USA.
⁵ Scilex Pharmaceuticals Inc., Mountain View, CA, USA.
⁶ Mid America PolyClinic, Overland Park, KS, USA.

Abstract

Purpose: This study compares the pharmacokinetic (PK) profile, adhesion, and safety of lidocaine topical system 1.8%, a novel lidocaine topical system approved to treat postherpetic neuralgia, under conditions of heat and exercise vs normal conditions.

Materials and methods: This open-label, 3-period, 3-treatment crossover study randomized 12 healthy adults to receive three lidocaine topical systems 1.8% during each of three treatment periods, with 7-day washouts between treatments. The product was applied to the mid-lower back and was removed after 12 hours. During Treatment A, subjects exercised on a bicycle for 30 minutes at 0, 2.5, 5.5, and 8.5 hours. During Treatment B, heat (temperature set at 36.7-40.3°C) was applied at 0 and 8.5 hours. Treatment C was normal conditions. The PK profile of each subject under exercise and heat conditions was compared to normal conditions. Skin irritation, adhesion, and adverse events were assessed.

Results: Twelve subjects completed the study. Exposure to external heat resulted in increased peak plasma concentration of lidocaine with a mean C_max of 160.3±100.1 ng/mL vs 97.6±36.9 ng/mL under normal conditions, with no effect on the extent of exposure (AUC). Concentrations returned to normal within 4 hours after the heat was removed. No clinically relevant differences in absorption were observed under exercise conditions with a mean C_max of 90.5±25.4 ng/mL and no effect on the extent (AUC) of lidocaine exposure was observed relative to normal conditions. No systems detached during the study. Adverse events were mild, with none leading to discontinuation.

Conclusion: Transient heat exposure resulted in increased lidocaine plasma concentrations compared to normal conditions, whereas exercise had no effect. The effects of heat appear to be immediate, reversible, and below systemic therapeutic threshold in antiarrhythmic treatment (1000-1500 ng/mL), and well below the safe systemic threshold of 5000 ng/mL. Lidocaine topical system 1.8% remained adhered to the skin and was well tolerated under all conditions. ClinicalTrials.gov: NCT04150536.

Keywords: dermal; herpes zoster; neuropathic pain; shingles.

Associated data

ClinicalTrials.gov/NCT04150536

Grants and funding

The project supported by Shandong Key Research and development Program (Grant No. 2018GSF118110).