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Triptorelin and cetrorelix induce immune responses and affect uterine development and expressions of genes and proteins of ESR1, LHR,and FSHR of mice
Authors:Suocheng Wei  Huiling Guo  Zhuandi Gong  Fengwei Zhang
Institution:1. Engineering &2. Technology Research Center of Animal Cells of Gansu Province, Northwest University for Nationalities, Lanzhou, China;3. Life Science and Engineering College, Northwest University for Nationalities, Lanzhou, China;4. Prevention and Control Center for Animal Diseases of Gansu Province, Lanzhou, China;5. Medicine College, Northwest University for Nationalities, Lanzhou, China;6. Life Science and Engineering College, Northwest University for Nationalities, Lanzhou, China
Abstract:Context: GnRH immunity can reduce the expression of pituitary GnRH levels, and cause the changes in reproductive behaviors. It is unclear whether triptorelin (TRI) and cetrorelix (CET) immunity influences uterine development and expression of follicle-stimulating hormone receptor (FSHR), luteinizing hormone receptor (LHR), and estradiol receptor 1 (ERS1) in the uterus.

Objective: The study investigated the effects of active immunity of GnRH agonist and antagonist on uterine development, microstructures, expression of hormone receptors mRNAs, and proteins in uteri.

Materials and methods: One hundred and five mice were assigned into CET, TRI, and control groups (CG). Mice in CET-1, CET-2, and CET-3 (n?=?15) were subcutaneously injected with 10, 20, and 40?μg CET antigens for seven days, respectively. Mice in TRI-1, TRI-2, and TRI-3 were injected with 10, 20, and 40?μg TRI antigens for seven days, respectively. The qPCR and Western blot were implemented to determine expressions of ESR1, LHR and FSHR mRNAs, and proteins.

Results: Compared with CG, the uterine weights of CET-1, CET-2, and CET-3 increased by 42.86, 62.86, and 10.00% on day 35 (p?p?p?p?p?Conclusions: CET immunity promoted the uterine development, improved EET and UWT, and also promoted the expressions of ESR1 and FSHR protein levels. It lessened the LHR protein levels. TRI immunity blocked EET and UWT, inhibited uterine growth and development. The efficacy of CET immunity was more obvious than TRI.
Keywords:Active immunity  cetrorelix  mice  microstructure  receptor  triptorelin  uterus
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