Abstract
Background: Animal and clinical studies have shown that remote ischemic conditioning (RIC) has protective effects for cerebral vascular diseases, with induced humoral factor changes in the peripheral blood. However, many findings are heterogeneous, perhaps due to differences in the RIC intervention schemes, enrolled populations, and sample times. This study aimed to examine the RIC-induced changes in the plasma proteome using rhesus monkey models of strokes. Methods: Two adult rhesus monkeys with autologous blood clot-induced middle cerebral artery (MCA) occlusion underwent RIC interventions twice a week for five consecutive weeks. Each RIC treatment included five cycles of five minutes of ischemia alternating with five minutes of reperfusion of the forearm. The blood samples were taken from the median cubital vein of the monkeys at baseline and immediately after each week’s RIC stimulus. The plasma samples were isolated for a proteomic analysis using mass spectrometry (MS). Results: Several proteins related to lipid metabolism (Apolipoprotein A-II and Apolipoprotein C-II), coagulation (Fibrinogen alpha chain and serpin), immunoinflammatory responses (complement C3 and C1), and endovascular hemostasis (basement membrane-specific heparan sulfate proteoglycan) were significantly modulated after the RIC intervention. Many of these induced changes, such as in the lipid metabolism regulation and anticoagulation responses, starting as early as two weeks following the RIC intervention. The complementary activation and protection of the endovascular cells occurred more than three weeks postintervention. Conclusions: Multiple protective effects were induced by RIC and involved lipid metabolism regulation (anti-atherogenesis), anticoagulation (antithrombosis), complement activation, and endovascular homeostasis (anti-inflammation). In conclusion, this study indicates that RIC results in significant modulations of the plasma proteome. It also provides ideas for future research and screening targets.
Highlights
Remote ischemic conditioning (RIC) is an extremely simple, noninvasive, and costeffective intervention
In terms of the upregulated proteins, the amount of proteins related to the “cellular process”, “biological regulation”, and metabolic process decreased two weeks after the remote ischemic conditioning (RIC) intervention, gradually climbed up during weeks three and four, and slightly decreased to a level that was lower than the baseline
We identified that Apolipoprotein A-II (Apo A-II) and Apolipoprotein C-II (Apo C-II) were upregulated after longterm RIC
Summary
Remote ischemic conditioning (RIC) is an extremely simple, noninvasive, and costeffective intervention. Former reviews have illustrated the multiorgan protective effect of RIC across the cardiovascular [1], renal [2], and cerebral systems [3]. Biomolecules 2021, 11, 1164 humoral, and immunological signaling pathways, which all interact with one another, appear to play requisite roles in the mechanisms that underlie the RIC-related beneficial effects [4]. We only found one prior animal study: Hibert et al observed seven major modulated proteins, including haptoglobin and transthyretin, after one RIC intervention (testing five-min vs. Animal and clinical studies have shown that remote ischemic conditioning (RIC) has protective effects for cerebral vascular diseases, with induced humoral factor changes in the peripheral blood. This study aimed to examine the RIC-induced changes in the plasma proteome using rhesus monkey models of strokes
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