The low‐expression programming of 11β‐HSD2 mediates osteoporosis susceptibility induced by prenatal caffeine exposure in male offspring rats

Xiao, Hao; Wu, Zhixin; Li, Bin; Shangguan, Yangfan; Stoltz, Jean‐François; Magdalou, Jacques; Chen, Liaobin; Wang, Hui

doi:10.1111/bph.15225

Cited by 18 publications

(8 citation statements)

References 49 publications

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“…Therefore, it is necessary to evaluate the expression stability of housekeeping genes in a specific model and select appropriate ones according to the actual situation. At present, the studies on fetal‐originated diseases are increasing (Liu et al, 2020; Xiao et al, 2020; Zhang et al, 2020), but the expression stability of housekeeping gene under the relevant models has not been comprehensively and systematically studied. DuBois et al found that the maternal low‐protein diet changed the expression levels of housekeeping genes in an age, sex, and organ‐dependent manner in rat offspring (DuBois et al, 2013).…”

Section: Discussionmentioning

confidence: 99%

The selection and identification of compound housekeeping genes for quantitative real‐time polymerase chain reaction analysis in rat fetal kidney

Zhao

Chen

Zhu

et al. 2021

J of Applied Toxicology

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During quantitative real‐time polymerase chain reaction (RT‐qPCR) data analysis, the selection of optimal housekeeping gene is necessary to ensure the accuracy of results. It is noteworthy that housekeeping genes commonly used in adult studies may not be applicable for fetus. However, the stability analysis of housekeeping gene in fetal kidney has not been reported. This study intends to screen the applicable compound housekeeping genes in rat fetal kidney. In this study, eight housekeeping genes used in kidney studies based on literature reports (GAPDH, ACTB, 18S, HPRT, YWHAZ, HMBS, PPIA, and TBP) were selected as the research object. Their expression levels in the rat fetal kidney in physiological condition and the intrauterine growth retardation (IUGR) model induced by prenatal dexamethasone exposure (PDE) (0.2 mg/kg·day from gestation Days 9 to 20) was measured. Furthermore, these eight housekeeping genes were used to conduct relative quantitative analysis of nephrin expression in the fetal kidney in PDE‐induced IUGR model, to compare the influence of choosing different housekeeping gene on data analysis of nephrin expression and to verify the reliability of selected compound housekeeping genes. In this study, stable housekeeping genes of fetal kidney tissues in PDE‐induced IUGR model were identified: ACTB, GAPDH, TBP, and HMBS for males; ACTB, YWHAZ, and GAPDH for females. Besides, our results suggest that ACTB + GAPDH were the best compound housekeeping genes for normalization analysis in male fetal kidney studies, and ACTB + YWHAZ in females. This study will provide an experimental evidence basis for the selection of housekeeping genes in the RT‐qPCR experiment in renal development toxicology‐related models.

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Section: Discussionmentioning

confidence: 99%

The selection and identification of compound housekeeping genes for quantitative real‐time polymerase chain reaction analysis in rat fetal kidney

Zhao

Chen

Zhu

et al. 2021

J of Applied Toxicology

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“…30 At 30 mg/kg•d, the changes of multiple indicators were significant, and there was a significant dose-dependent relationship with different doses of 30, 60, and 120 mg/kg•d. [30][31][32] Therefore, to fully reflect the developmental toxicity of caffeine and obtain a stable IUGR model, we used a maximum concentration of 120 mg/kg•d caffeine in this study. Thus, caffeine concentrations of 30, 60, and 120 mg/kg•d were selected for the animal experiment in this study.…”

Section: Rationality and Significance Of Caffeine Doses And Fetal Rats Gender Used In This Studymentioning

confidence: 87%

Prenatal caffeine exposure caused H‐type blood vessel‐related long bone dysplasia via miR375/CTGF signaling

Luo

et al. 2021

FASEB j.

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Caffeine has developmental toxicity. Prenatal caffeine exposure (PCE) caused intrauterine growth retardation (IUGR) and multiple organ dysplasia. This study intended to explore the effect and mechanism of PCE on long bone development in female fetal rats. In vivo, the PCE group pregnant rats were given different concentrations of caffeine during the gestational Day 9-20. The mRNA expression of osteogenesis-related genes were significantly reduced in PCE group. In the PCE group (120 mg/kg•d), the length and primary center of fetal femur were shorter, and accompanied by H-type blood vessel abundance reducing. Meanwhile, connective tissue growth factor (CTGF) expression decreased in the growth plate of the PCE group (120 mg/kg•d). In contrast, the miR375 expression increased. In vitro, caffeine decreased CTGF and increased miR375 expression in fetal growth plate chondrocytes.After co-culture with caffeine-treated chondrocytes, the tube formation ability for the H-type endothelial cells was decreased. Furthermore, CTGF overexpression or miR375 inhibitor reversed caffeine-induced reduction of tube formation ability, and miR375 inhibitor reversed caffeine-induced CTGF expression inhibition. In summary, PCE decreased the expression of CTGF by miR375, ultimately resulting in H-type blood vessel-related long bone dysplasia. K E Y W O R D Sbone dysplasia, connective tissue growth factor, H-type blood vessel, microRNA375, prenatal caffeine exposure 2 of 13 | HE Et al. How to cite this article: He H, Luo H, Liu L, et al. Prenatal caffeine exposure caused H-type blood vessel-related long bone dysplasia via miR375/CTGF signaling.

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“…( Figure 1 ) In addition, a recent study shows that HDAC11 contributes to osteoporosis susceptibility and reduced peak bone mass through a mechanism of 11β-HSD2’s low-functional programming. This is triggered by corticosterone through GR/HDAC11 signaling, which amplifies the effect of corticosterone on inhibiting the function of BMSCs in osteogenesis ( 141 , 142 ). However, studies on diabetic osteoporosis, lipoid nephrosis, fatty liver disease and obesity cardiomyopathy are still lacking.…”

Section: Discussionmentioning

confidence: 99%

HDAC11, an emerging therapeutic target for metabolic disorders

et al. 2022

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Histone deacetylase 11 (HDAC11) is the only member of the class IV HDAC, and the latest member identified. It is highly expressed in brain, heart, kidney and some other organs, and located in mitochondria, cytoplasm and nuclei, depending on the tissue and cell types. Although studies in HDAC11 total knockout mice suggest its dispensable features for tissue development and life, it participates in diverse pathophysiological processes, such as DNA replication, tumor growth, immune regulation, oxidant stress injury and neurological function of cocaine. Recent studies have shown that HDAC11 is also critically involved in the pathogenesis of some metabolic diseases, including obesity, diabetes and complications of diabetes. In this review, we summarize the recent progress on the role and mechanism of HDAC11 in the regulation of metabolic disorders, with the focus on its regulation on adipogenesis, lipid metabolism, metabolic inflammation, glucose tolerance, immune responses and energy consumption. We also discuss the property and selectivity of HDAC11 inhibitors and their applications in a variety of in vitro and in vivo models of metabolic disorders. Given that pharmacological and genetic inhibition of HDAC11 exerts a beneficial effect on various metabolic disorders, HDAC11 may be a potential therapeutic target to treat chronic metabolic diseases.

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The low‐expression programming of 11β‐HSD2 mediates osteoporosis susceptibility induced by prenatal caffeine exposure in male offspring rats

Cited by 18 publications

References 49 publications

The selection and identification of compound housekeeping genes for quantitative real‐time polymerase chain reaction analysis in rat fetal kidney

The selection and identification of compound housekeeping genes for quantitative real‐time polymerase chain reaction analysis in rat fetal kidney

Prenatal caffeine exposure caused H‐type blood vessel‐related long bone dysplasia via miR375/CTGF signaling

HDAC11, an emerging therapeutic target for metabolic disorders

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