Autor: |
Morena F; Department of Health, Human Performance and Recreation, University of Arkansas at Fayetteville, Fayetteville, AR, United States., Cabrera AR; Department of Health, Human Performance and Recreation, University of Arkansas at Fayetteville, Fayetteville, AR, United States., Jones Iii RG; Health, Human Performance, and Recreation, University of Arkansas, Fayetteville, AR, United States., Schrems ER; Department of Health, Human Performance and Recreation, University of Arkansas at Fayetteville, Fayetteville, AR, United States., Muhyudin R; Department of Health, Human Performance and Recreation, University of Arkansas at Fayetteville, Fayetteville, AR, United States., Washington TA; Department of Health, Human Performance, and Recreation, University of Arkansas at Fayetteville, Fayetteville, AR, United States., Murach KA; Department of Health, Human Performance and Recreation, University of Arkansas at Fayetteville, Fayetteville, AR, United States., Greene NP; Department of Health, Human Performance and Recreation, University of Arkansas at Fayetteville, Fayetteville, AR, United States. |
Abstrakt: |
Studies suggest heterogeneity in cancer cachexia (CC) among models and biological sexes, yet examinations comparing models and sexes are scarce. We compared the transcriptional landscape of skeletal muscle across murine CC models and biological sexes during early and late CC. Global gene expression analyses were performed on gastrocnemius (LLC-Lewis Lung Carcinoma), quadriceps (KPC-pancreatic), and tibialis anterior (C26-colorectal and Apc Min/+ ) muscles across biological sexes. Differentially expressed genes (DEGs) were identified using an adj-p-value of <0.05, followed by pathway and computational cistrome analyses. Integrating all controls, early, and late-stage of all models and sexes revealed up to 68% of DEGs and pathways were enriched at early and late CC, indicating a conserved transcriptional profile during CC development. Comparing DEGs and pathways within sexes and across models, in early-CC, the transcriptional response was highly heterogeneous. At late-stage, 11.5% of upregulated and 10% of downregulated genes were shared between models in males, while 18.9% of upregulated and 7% of downregulated DEGs were shared in females. Shared DEGs were enriched in proteasome and mitophagy/autophagy pathways (upregulated), and downregulation of energy metabolism pathways in males only. Between sexes, though proportion of shared DEGs was low (<16%), similar pathway enrichment was observed, including proteasome and mitophagy at late-stage CC. In early-CC, Osmr upregulation was the only commonality across all models and sexes, while CLOCK and ARNTL/BMAL1 were predicted transcriptional factors associated with dysregulations in all three male models. This study highlights sex and model differences in CC progression and suggests conserved transcriptional changes as potential therapeutic targets. |