Plasma proteome profiling reveals the therapeutic effects of the PPAR pan-agonist chiglitazar on insulin sensitivity, lipid metabolism, and inflammation in type 2 diabetes

Jan 5, 2024Scientific reports

Blood protein patterns show how chiglitazar improves insulin use, fat metabolism, and inflammation in type 2 diabetes

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Abstract

Of the 157 patients studied, 13 proteins were associated with chiglitazar treatment.

  • Ten proteins were found to be up-regulated after chiglitazar treatment, indicating potential benefits in insulin sensitivity and lipid metabolism.
  • Three proteins were down-regulated following treatment, which may relate to inflammation response.
  • The specific proteins identified include SHBG, TF, APOA2, and APOA1 among the up-regulated and PRG4, FETUB, and C2 among the down-regulated.
  • Plasma proteome profiling was conducted at baseline and at 12 and 24 weeks post-treatment using advanced mass spectrometry.
  • Chiglitazar has been newly approved in China for use as an adjunct to diet and exercise in managing glycemic control in adults with Type 2 Diabetes.

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Key numbers

10
Proteins Upregulated
Proteins associated with insulin sensitivity and lipid metabolism.
3
Proteins Downregulated
Proteins linked to glucose regulation and metabolic control.
314
Total Proteins Analyzed
Proteins profiled across treatment groups in the study.

Full Text

What this is

  • Chiglitazar is a novel approved in China for treating ().
  • This study profiles plasma proteomes to assess the effects of chiglitazar on insulin sensitivity, lipid metabolism, and inflammation in patients.
  • 157 patients were treated with chiglitazar, sitagliptin, or placebo, with plasma samples collected at baseline and after 12 and 24 weeks.

Essence

  • Chiglitazar treatment in patients significantly altered 13 plasma proteins, enhancing insulin sensitivity and lipid metabolism while modulating inflammation. Notable changes included upregulation of proteins like SHBG and APOA1, indicating potential therapeutic benefits.

Key takeaways

  • Chiglitazar treatment resulted in 10 proteins being upregulated, including SHBG, which is linked to improved insulin sensitivity. This change suggests a positive effect on glucose regulation in patients.
  • Three proteins were downregulated after chiglitazar treatment, including FETUB, which is associated with insulin sensitivity. This downregulation may further support chiglitazar's role in enhancing metabolic control.
  • Chiglitazar demonstrated multi-faceted effects by regulating proteins involved in inflammation and lipid metabolism, potentially offering additional benefits beyond glucose control in management.

Caveats

  • The study's findings are based on a specific patient population, which may limit generalizability. Further research is needed to confirm these results in diverse cohorts.
  • The study relies on proteomic profiling, which may not capture all relevant biological changes. Additional studies are necessary to elucidate the comprehensive mechanisms of chiglitazar's effects.

Definitions

  • Type 2 Diabetes (T2D): A chronic metabolic disorder characterized by insulin resistance and high blood glucose levels.
  • PPAR pan-agonist: A compound that activates all three types of peroxisome proliferator-activated receptors (α, β/δ, and γ), targeting multiple metabolic pathways.

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