Heterogeneity in heat shock response dynamics caused by translation fidelity decline and proteostasis collapse

Vertti-Quintero, Nadia; Berger, Simon; Solvas, Xavier Casadevall i; Statzer, Cyril; Annis, Jillian; Ruppen, Peter; Stavrakis, Stavros; Ewald, Collin Y.; deMello, Andrew J.

doi:10.1101/822072

Cited by 2 publications

(1 citation statement)

References 72 publications

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“…We observed tissue-specific gene ontology (GO) enrichment of the best longevity correlated genes (Figure 3 and Supplementary Table 3). These include several processes known to be vital to promote healthy aging, such as immune responses, neuronal signaling, heat shock proteins, epigenetic reprogramming, extracellular matrix, and mitochondrial energy metabolism (Figure 3; Greer et al, 2011;Houtkooper et al, 2013;López-Otín et al, 2013;Ewald et al, 2015;Denzel et al, 2019;Ewald, 2019;Hess et al, 2019;Vertti-Quintero et al, 2019;Gallotta et al, 2020). For instance, the adrenal gland showed enrichment for immune responses, whereas in the liver, oxidative phosphorylation and mitochondrial components were enriched (Figure 3).…”

Section: Gene Expression Correlating With Lifespanmentioning

confidence: 99%

Lifespan-Associated Gene Expression Signatures of Recombinant BXD Mice Implicates Coro7 and Set in Longevity

et al. 2021

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Although genetic approaches have identified key genes and pathways that promote longevity, systems-level approaches are less utilized. Here, we took advantage of the wealth of omics data characterizing the BXD family of mice. We associated transcript and peptide levels across five tissues from both female and male BXD isogenic lines with their median lifespan. We identified over 5000 genes that showed a longevity correlation in a given tissue. Surprisingly, we found less than 1% overlap among longevity-correlating genes across tissues and sex. These 1% shared genes consist of 51 genes, of which 13 have been shown to alter lifespan. Only two genes -Coro7 and Set- showed a longevity correlation in all tissues and in both sexes. While differential regulation of aging across tissues and sex has been reported, our systems-level analysis reveals two unique genes that may promote healthy aging in unique sex- and tissue-agnostic manner.

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Section: Gene Expression Correlating With Lifespanmentioning

confidence: 99%

Lifespan-Associated Gene Expression Signatures of Recombinant BXD Mice Implicates Coro7 and Set in Longevity

et al. 2021

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3D mechanical characterization of single cells and small organisms using acoustic manipulation and force microscopy

et al. 2021

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Quantitative micromechanical characterization of single cells and multicellular tissues or organisms is of fundamental importance to the study of cellular growth, morphogenesis, and cell-cell interactions. However, due to limited manipulation capabilities at the microscale, systems used for mechanical characterizations struggle to provide complete three-dimensional coverage of individual specimens. Here, we combine an acoustically driven manipulation device with a micro-force sensor to freely rotate biological samples and quantify mechanical properties at multiple regions of interest within a specimen. The versatility of this tool is demonstrated through the analysis of single Lilium longiflorum pollen grains, in combination with numerical simulations, and individual Caenorhabditis elegans nematodes. It reveals local variations in apparent stiffness for single specimens, providing previously inaccessible information and datasets on mechanical properties that serve as the basis for biophysical modelling and allow deeper insights into the biomechanics of these living systems.

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Heterogeneity in heat shock response dynamics caused by translation fidelity decline and proteostasis collapse

Cited by 2 publications

References 72 publications

Lifespan-Associated Gene Expression Signatures of Recombinant BXD Mice Implicates Coro7 and Set in Longevity

Lifespan-Associated Gene Expression Signatures of Recombinant BXD Mice Implicates Coro7 and Set in Longevity

3D mechanical characterization of single cells and small organisms using acoustic manipulation and force microscopy

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