AI Article Synopsis

  • - Tinnitus is characterized by hearing sounds that aren't there, and its causes and potential treatments are still not fully understood.
  • - A study on rats analyzed gene changes in the brain region linked to hearing after inducing tinnitus, finding 87 genes that were either increased or decreased in expression.
  • - Pathway analysis indicated links to conditions like COVID-19 and identified key genes (Rpl7a and AC136661.1) that could be targeted for future treatment strategies in tinnitus.

Article Abstract

Tinnitus is a disturbing condition defined as the occurrence of acoustic hallucinations with no actual sound. Although the mechanisms underlying tinnitus have been explored extensively, the pathophysiology of the disease is not completely understood. Moreover, genes and potential treatment targets related to auditory hallucinations remain unknown. In this study, we examined transcriptional-profile changes in the medial geniculate body after noise-induced tinnitus in rats by performing RNA sequencing and validated differentially expressed genes via quantitative polymerase chain reaction analysis. The rat model of tinnitus was established by analyzing startle behavior based on gap-pre-pulse inhibition of acoustic startles. We identified 87 differently expressed genes, of which 40 were upregulated and 47 were downregulated. Pathway-enrichment analysis revealed that the differentially enriched genes in the tinnitus group were associated with pathway terms, such as coronavirus disease COVID-19, neuroactive ligand-receptor interaction. Protein-protein-interaction networks were established, and two hub genes (Rpl7a and AC136661.1) were identified among the selected genes. Further studies focusing on targeting and modulating these genes are required for developing potential treatments for noise-induced tinnitus in patients.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10984379PMC
http://dx.doi.org/10.3389/ebm.2024.10057DOI Listing

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