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Abstract TP274: Orosomucoid-1 Protein Increases Following Ischemic Stroke in the Brain and Periphery
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Background and Purpose:
Orosomucoid-1 (ORM-1) is an abundant protein with important roles in inflammation and immunosuppression. We utilized RNA sequencing to measure mRNA levels in human ischemic stroke patients, with confirmation by serum ORM-1 protein measurements. A mouse model of ischemic stroke was then used to examine post-stroke changes in ORM-1 within the brain itself.
Hypothesis:
We tested the hypothesis that ORM-1 levels increase following ischemic stroke, with sex differences in protein dynamics over time.
Methods:
RNA sequencing was performed on whole blood from ischemic stroke patients (n=23) and controls (n=12), with Benjamini-Hochberg correction for multiple testing. Enzyme-linked immunosorbent assay was performed on serum from ischemic stroke patients (n=28) and controls (n=8), with analysis by T-test. For brain analysis, mice (n=14) were subjected to a 90-minute middle cerebral artery occlusion (MCAO) surgery and sacrificed 6 or 24 hours after stroke. Control mice underwent parallel “sham” surgery without occlusion. Western blotting was used to detect ORM-1 protein levels in whole brain, with analysis by two-way ANOVA.
Results:
RNA sequencing showed a 2.8-fold increase in human ORM-1 at 24 hours post-stroke (q=.0029), an increase also seen in serum ORM-1 protein levels (p=.011). Western blot analysis of mouse brain revealed that glycosylated (p=0.0003) and naive (p=0.0333) forms of ORM-1 were higher in female mice compared to males 6 hours post-stroke. Interestingly, ORM-1 levels were higher in the brains of stroke mice at 6 hours (p=.0483), while at 24 hours ORM-1 levels in stroke mice were lower than their sham counterparts (p=.0212). In both human and mouse data, no sex differences were seen in ORM-1 levels in the brain or periphery at 24 hours post-stroke.
Conclusion:
In conclusion, ORM-1 is a sexually dimorphic protein involved in the early (<24 hour) response to ischemic stroke. This research serves as an initial step in determining the mechanism of ORM-1 in the ischemic stroke response and its potential as a future therapeutic target for both sexes.
Ovid Technologies (Wolters Kluwer Health)
Title: Abstract TP274: Orosomucoid-1 Protein Increases Following Ischemic Stroke in the Brain and Periphery
Description:
Background and Purpose:
Orosomucoid-1 (ORM-1) is an abundant protein with important roles in inflammation and immunosuppression.
We utilized RNA sequencing to measure mRNA levels in human ischemic stroke patients, with confirmation by serum ORM-1 protein measurements.
A mouse model of ischemic stroke was then used to examine post-stroke changes in ORM-1 within the brain itself.
Hypothesis:
We tested the hypothesis that ORM-1 levels increase following ischemic stroke, with sex differences in protein dynamics over time.
Methods:
RNA sequencing was performed on whole blood from ischemic stroke patients (n=23) and controls (n=12), with Benjamini-Hochberg correction for multiple testing.
Enzyme-linked immunosorbent assay was performed on serum from ischemic stroke patients (n=28) and controls (n=8), with analysis by T-test.
For brain analysis, mice (n=14) were subjected to a 90-minute middle cerebral artery occlusion (MCAO) surgery and sacrificed 6 or 24 hours after stroke.
Control mice underwent parallel “sham” surgery without occlusion.
Western blotting was used to detect ORM-1 protein levels in whole brain, with analysis by two-way ANOVA.
Results:
RNA sequencing showed a 2.
8-fold increase in human ORM-1 at 24 hours post-stroke (q=.
0029), an increase also seen in serum ORM-1 protein levels (p=.
011).
Western blot analysis of mouse brain revealed that glycosylated (p=0.
0003) and naive (p=0.
0333) forms of ORM-1 were higher in female mice compared to males 6 hours post-stroke.
Interestingly, ORM-1 levels were higher in the brains of stroke mice at 6 hours (p=.
0483), while at 24 hours ORM-1 levels in stroke mice were lower than their sham counterparts (p=.
0212).
In both human and mouse data, no sex differences were seen in ORM-1 levels in the brain or periphery at 24 hours post-stroke.
Conclusion:
In conclusion, ORM-1 is a sexually dimorphic protein involved in the early (<24 hour) response to ischemic stroke.
This research serves as an initial step in determining the mechanism of ORM-1 in the ischemic stroke response and its potential as a future therapeutic target for both sexes.
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