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Lipidized Prolactin-Releasing Peptide as a New Potential Tool to Treat Obesity and Type 2 Diabetes Mellitus: Preclinical Studies in Rodent Models

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    SYSNO ASEP0552394
    Document TypeJ - Journal Article
    R&D Document TypeJournal Article
    Subsidiary JČlánek ve WOS
    TitleLipidized Prolactin-Releasing Peptide as a New Potential Tool to Treat Obesity and Type 2 Diabetes Mellitus: Preclinical Studies in Rodent Models
    Author(s) Mráziková, L. (CZ)
    Neprašová, Barbora (FGU-C)
    Mengr, A. (CZ)
    Popelová, A. (CZ)
    Strnadová, V. (CZ)
    Holá, L. (CZ)
    Železná, B. (CZ)
    Kuneš, Jaroslav (FGU-C) RID, ORCID
    Maletínská, L. (CZ)
    Article number779962
    Source TitleFrontiers in Pharmacology. - : Frontiers Media - ISSN 1663-9812
    Roč. 12, Nov 18 (2021)
    Number of pages11 s.
    Languageeng - English
    CountryCH - Switzerland
    Keywordsprolactin-releasing peptide ; rodent models ; obesity ; type 2 diabetes ; leptin resistance
    OECD categoryPhysiology (including cytology)
    R&D ProjectsGA21-03691S GA ČR - Czech Science Foundation (CSF)
    Method of publishingOpen access
    Institutional supportFGU-C - RVO:67985823
    UT WOS000765086400001
    EID SCOPUS85120610055
    DOI10.3389/fphar.2021.779962
    AnnotationObesity and type 2 diabetes mellitus (T2DM) are preconditions for the development of metabolic syndrome, which is reaching pandemic levels worldwide, but there are still only a few anti-obesity drugs available. One of the promising tools for the treatment of obesity and related metabolic complications is anorexigenic peptides, such as prolactin-releasing peptide (PrRP). PrRP is a centrally acting neuropeptide involved in food intake and body weight (BW) regulation. In its natural form, it has limitations for peripheral administration, thus, we designed analogs of PrRP lipidized at the N-terminal region that showed high binding affinities, increased stability and central anorexigenic effects after peripheral administration. In this review, we summarize the preclinical results of our chronic studies on the pharmacological role of the two most potent palmitoylated PrRP31 analogs in various mouse and rat models of obesity, glucose intolerance, and insulin resistance. We used mice and rats with diet-induced obesity fed a high-fat diet, which is considered to simulate the most common form of human obesity, or rodent models with leptin deficiency or disrupted leptin signaling in which long-term food intake regulation by leptin is distorted. The rodent models described in this review are models of metabolic syndrome with different severities, such as obesity or morbid obesity, prediabetes or diabetes and hypertension. We found that the effects of palmitoylated PrRP31 on food intake and BW but not on glucose intolerance require intact leptin signaling. Thus, palmitoylated PrRP31 analogs have potential as therapeutics for obesity and related metabolic complications.
    WorkplaceInstitute of Physiology
    ContactLucie Trajhanová, lucie.trajhanova@fgu.cas.cz, Tel.: 241 062 400
    Year of Publishing2022
    Electronic addresshttps://doi.org/10.3389/fphar.2021.779962
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