A Pseudo‐Surfactant Chemical Permeation Enhancer to Treat Otitis Media via Sustained Transtympanic Delivery of Antibiotics

Author:

Liu Sophie S.12ORCID,White Joanna M.3ORCID,Chao Zhongmou1ORCID,Li Ruye4ORCID,Wen Shuxian1ORCID,Garza Ally5ORCID,Tang Wenjing1,Ma Xiaojing1,Chen Pengyu1,Daniel Susan1ORCID,Bates Frank S.3ORCID,Yeo Jingjie6ORCID,Calabrese Michelle A.3ORCID,Yang Rong1ORCID

Affiliation:

1. Robert F. Smith School of Chemical and Biomolecular Engineering Cornell University Olin Hall Ithaca NY 14850 USA

2. Meinig School of Biomedical Engineering Cornell University Weill Hall Ithaca NY 14850 USA

3. Department of Chemical Engineering and Materials Science University of Minnesota 421 Washington Ave. Minneapolis MN 55455 USA

4. Department of Chemistry and Chemical Biology Cornell University Baker Laboratory Ithaca NY 14850 USA

5. Department of Health and Biomedical Sciences University of Texas Rio Grande Valley 1201 W University Drive Edinburg TX 78539 USA

6. Sibley School of Mechanical and Aerospace Engineering Cornell University Upson Hall Ithaca NY 14850 USA

Abstract

AbstractChemical permeation enhancers (CPEs) represent a prevalent and safe strategy to enable noninvasive drug delivery across skin‐like biological barriers such as the tympanic membrane (TM). While most existing CPEs interact strongly with the lipid bilayers in the stratum corneum to create defects as diffusion paths, their interactions with the delivery system, such as polymers forming a hydrogel, can compromise gelation, formulation stability, and drug diffusion. To overcome this challenge, differing interactions between CPEs and the hydrogel system are explored, especially those with sodium dodecyl sulfate (SDS), an ionic surfactant and a common CPE, and those with methyl laurate (ML), a nonionic counterpart with a similar length alkyl chain. Notably, the use of ML effectively decouples permeation enhancement from gelation, enabling sustained delivery across TMs to treat acute otitis media (AOM), which is not possible with the use of SDS. Ciprofloxacin and ML are shown to form a pseudo‐surfactant that significantly boosts transtympanic permeation. The middle ear ciprofloxacin concentration is increased by 70‐fold in vivo in a chinchilla AOM model, yielding superior efficacy and biocompatibility than the previous highest‐performing formulation. Beyond improved efficacy and biocompatibility, this single‐CPE formulation significantly accelerates its progression toward clinical deployment.

Funder

Natural Sciences and Engineering Research Council of Canada

National Science Foundation

National Science Foundation Graduate Research Fellowship Program

National Institute on Deafness and Other Communication Disorders

Publisher

Wiley

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