Anti-inflammatory Therapy Protects Spiral Ganglion Neurons After Aminoglycoside Antibiotic-Induced Hair Cell Loss

被引:0
作者
Muhammad T. Rahman
Erin M. Bailey
Benjamin M. Gansemer
Andrew A. Pieper
J. Robert Manak
Steven H. Green
机构
[1] University of Iowa,Department of Biology
[2] University Hospitals Cleveland Medical Center,Harrington Discovery Institute
[3] Case Western Reserve University,Department of Psychiatry
[4] Geriatric Psychiatry,Institute for Transformative Molecular Medicine, School of Medicine
[5] GRECC,Department of Pediatrics
[6] Louis Stokes Cleveland VA Medical Center,undefined
[7] Case Western Reserve University,undefined
[8] University of Iowa,undefined
来源
Neurotherapeutics | 2023年 / 20卷
关键词
Neurodegeneration; Deafening; Inflammation; Dexamethasone; Ibuprofen; P7C3-A20;
D O I
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学科分类号
摘要
Destruction of cochlear hair cells by aminoglycoside antibiotics leads to gradual death of the spiral ganglion neurons (SGNs) that relay auditory information to the brain, potentially limiting the efficacy of cochlear implants. Because the reasons for this cochlear neurodegeneration are unknown, there are no neuroprotective strategies for patients. To investigate this problem, we assessed transcriptomic changes in the rat spiral ganglion following aminoglycoside antibiotic (kanamycin)-induced hair cell destruction. We observed selectively increased expression of immune and inflammatory response genes and increased abundance of activated macrophages in spiral ganglia by postnatal day 32 in kanamycin-deafened rats, preceding significant SGN degeneration. Treatment with the anti-inflammatory medications dexamethasone and ibuprofen diminished long-term SGN degeneration. Ibuprofen and dexamethasone also diminished macrophage activation. Efficacy of ibuprofen treatment was augmented by co-administration of the nicotinamide adenine dinucleotide-stabilizing agent P7C3-A20. Our results support a critical role of neuroinflammation in SGN degeneration after aminoglycoside antibiotic-mediated cochlear hair cell loss, as well as a neuroprotective strategy that could improve cochlear implant efficacy.
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页码:578 / 601
页数:23
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