Background <p>The cyclin-dependent kinase inhibitor <i>CDKN2A/p16INK4A</i> (<i>p16INK4A</i>) is a central regulator of cellular senescence, widely studied in ageing and cancer. Although its expression increases with age and disease, its role in the adult brain remains poorly defined. Recent evidence suggests a possible contribution to neuroinflammation and cognitive decline in Alzheimer’s disease (AD), but underlying mechanisms are unclear. We investigated the functional impact of <i>p16Ink4a</i> inactivation on spatial cognition and hippocampal gene expression in adult mice under normal and amyloidogenic conditions using the <i>App</i><sup><i>NL−G−F</i></sup> AD model.</p> Methods <p>Spatial learning and memory were assessed using the Morris Water Maze (MWM). Hippocampal transcriptomes from control, <i>p16INK4A</i><sup><i>knockout</i></sup> (<i>p16Ink4a</i><sup><i>KO</i></sup>), <i>App</i><sup><i>NL−G−F</i></sup>, and double mutant mice were analysed by RNA sequencing. We performed differential gene expression analysis, gene set enrichment analysis (GSEA), and interaction modelling to assess the molecular consequences of <i>p16Ink4a</i> loss alone and in combination with amyloid pathology.</p> Results <p>Loss of <i>p16Ink4a</i> resulted in modest and short-lasting alterations in spatial learning and early memory retrieval, without exacerbating early deficits in <i>App</i><sup><i>NL−G−F</i></sup> mice. Transcriptomic analysis indicated that <i>p16Ink4a</i><sup><i>KO</i></sup> upregulated metabolic, mitochondrial, and translational pathways, while downregulating synaptic and cytoskeletal genes. In contrast, <i>App</i><sup><i>NL−G−F</i></sup> mice displayed strong immune activation. The double mutants showed additive transcriptional changes, yet GSEA indicated non-linear interactions in synaptic and immune-related pathways. Unexpectedly, <i>p16Ink4a</i> deletion alone was associated with enrichment of senescence-related signatures.</p> Conclusion <p>Constitutive <i>p16Ink4a</i> loss shows modest effects on spatial memory and broad hippocampal transcriptomic changes, independently of amyloid pathology. These findings point to possible non-canonical roles for <i>p16Ink4a</i> in neuronal homeostasis and emphasise the need for temporally controlled models to better dissect the brain-specific functions of senescence regulators in ageing and neurodegeneration.</p>

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Cdkn2a/p16Ink4a loss impairs Spatial memory independently of Alzheimer’s-associated genetic pathways in young adult mice

  • Pauline Stephan,
  • Damien Plassard,
  • William M. Keyes,
  • Yann Hérault

摘要

Background

The cyclin-dependent kinase inhibitor CDKN2A/p16INK4A (p16INK4A) is a central regulator of cellular senescence, widely studied in ageing and cancer. Although its expression increases with age and disease, its role in the adult brain remains poorly defined. Recent evidence suggests a possible contribution to neuroinflammation and cognitive decline in Alzheimer’s disease (AD), but underlying mechanisms are unclear. We investigated the functional impact of p16Ink4a inactivation on spatial cognition and hippocampal gene expression in adult mice under normal and amyloidogenic conditions using the AppNL−G−F AD model.

Methods

Spatial learning and memory were assessed using the Morris Water Maze (MWM). Hippocampal transcriptomes from control, p16INK4Aknockout (p16Ink4aKO), AppNL−G−F, and double mutant mice were analysed by RNA sequencing. We performed differential gene expression analysis, gene set enrichment analysis (GSEA), and interaction modelling to assess the molecular consequences of p16Ink4a loss alone and in combination with amyloid pathology.

Results

Loss of p16Ink4a resulted in modest and short-lasting alterations in spatial learning and early memory retrieval, without exacerbating early deficits in AppNL−G−F mice. Transcriptomic analysis indicated that p16Ink4aKO upregulated metabolic, mitochondrial, and translational pathways, while downregulating synaptic and cytoskeletal genes. In contrast, AppNL−G−F mice displayed strong immune activation. The double mutants showed additive transcriptional changes, yet GSEA indicated non-linear interactions in synaptic and immune-related pathways. Unexpectedly, p16Ink4a deletion alone was associated with enrichment of senescence-related signatures.

Conclusion

Constitutive p16Ink4a loss shows modest effects on spatial memory and broad hippocampal transcriptomic changes, independently of amyloid pathology. These findings point to possible non-canonical roles for p16Ink4a in neuronal homeostasis and emphasise the need for temporally controlled models to better dissect the brain-specific functions of senescence regulators in ageing and neurodegeneration.