ACTH-like Peptides Compensate Rat Brain Gene Expression Profile Disrupted by Ischemia a Day After Experimental Stroke.

Biomedicines2024PMID: 39767736

View on PubMed DOI: 10.3390/biomedicines12122830

Animal StudySemax

Plain Language Summary

At 24 hours after experimental stroke in rats, Semax and a related peptide (ACTH(6-9)PGP) both significantly normalized the expression of nearly 1,200 genes disrupted by ischemia, particularly those involved in immune signaling and neural communication. This transcriptome-level protection aligned with previously observed structural protection in brain tissue. Comparing effects at 4.5 hours versus 24 hours shows the peptides' gene-level influence shifts over time, which has implications for identifying the best treatment window.

Abstract

Ischemic stroke results from a disruption of cerebral blood flow. Adrenocorticotropic hormone (ACTH) serves as the basis for the creation of synthetic peptides as neuroprotective agents for stroke therapy. Previously, using RNA-Seq we first revealed differential expressed genes (DEGs) associated with ACTH(4-7)PGP (Semax) and ACTH(6-9)PGP peptides under cerebral ischemia conditions. Analysis was carried out at 4.5 h after transient middle cerebral artery occlusion (tMCAO) model in the ipsilateral frontal cortex of a rat brain.Here, we analyzed the penumbra-associated frontal cortex of rats and actions under the same peptides at 24 h after tMCAO using RNA-Seq.3774 DEGs (fold change > 1.5 and< 0.05) were identified under ischemia conditions, whereas 1539 and 2066 DEGs were revealed under Semax and ACTH(6-9)PGP peptides at 24 h after tMCAO. Furthermore, both peptides significantly reduced expression distortions caused by ischemia for 1171 genes associated with immune and neurosignaling pathways. Concomitantly, there were 32 DEGs under ACTH(6-9)PGP versus Semax administration at 24 h after tMCAO. Besides, neurogenesis-, angiogenesis-, protein kinase- and growth factor-related DEGs were revealed under peptides action. Previously, we observed the neuroprotective effect of peptides at the histological level in rat brains at 24 h after tMCAO. Thus, here we demonstrate the transcriptome manifestation of this histological effect. Furthermore, comparison with previous data at the 4.5 h post-tMCAO time point showed that the pattern of peptide action on the transcriptome depends on the time elapsed after tMCAO.We revealed that the effect of ACTH(6-9)PGP was more similar to Semax than different from it a day after tMCAO. At this time point, ACTH-like peptides compensated rat brain gene expression profiles disrupted by ischemia. Thus, our results may be useful for selecting more effective structures for future anti-stroke drugs and appropriate post-stroke time points for their testing.

Authors

Filippenkov, Ivan B; Shpetko, Yana Yu; Stavchansky, Vasily V; Denisova, Alina E; Gubsky, Leonid V; Andreeva, Lyudmila A; Myasoedov, Nikolay F; Limborska, Svetlana A; Dergunova, Lyudmila V

Keywords

ACTH(4–7)PGP (Semax)ACTH(6–9)PGPRNA-Seqdifferential expressed genesgene networkischemic stroke