Accelerated age-related decline in hippocampal neurogenesis in mice with noise-induced hearing loss is associated with hippocampal microglial degeneration

Hong Zhuang; Jing Yang; Zhihui Huang; Haiqing Liu; Xiaobo Li; Hongyu Zhang; Jiadong Wang; Shen Yu; Kefei Liu; Rui Liu; Mingze Bi; Jian Wang; Richard J. Salvi; Bohua Hu; Gaojun Teng; Lijie Liu

doi:doi:10.18632/aging.103898

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Research Paper Volume 12, Issue 19 pp 19493—19519

Accelerated age-related decline in hippocampal neurogenesis in mice with noise-induced hearing loss is associated with hippocampal microglial degeneration

NIHL mice exhibited an accelerated age-related decline in hippocampal neurogenesis. (A–J) Representative images of Ki67⁺ (green) and DCX⁺ (red) cells in the hippocampal DG of control and NIHL mice at 4 DPN (A, F), 1 MPN (B, G), 3 MPN (C, H), 6 MPN (D, I) and 12 MPN (E, J). Note the accumulation of autofluorescent lipofuscin deposits (red), a sign of normal senescence [43], in the DG of control and NIHL mice at 6 MPN and 12 MPN. Scale bar: 100 μm. (K, L) Enlarged views of B (K, flipped horizontally) and G (L). Arrowheads indicate Ki67⁺ (green) cells. Asterisks and arrows in the magnified inserts indicate the soma and processes of DCX⁺ cells (red). Note the obvious reduction in branch complexity of DCX⁺ cells in NIHL mice. Scale bar: 100 μm. (M, N) Quantitative analyses of Ki67⁺ cells (M) and DCX⁺ cells (N) in the DG of mice at different time points. **P<0.01, ***P<0.001 (two-way ANOVA, post hoc Tukey’s test, vs. age-matched control group).