Your search keyword '"Jiang, Juntao"' showing total 4 results

1. Study on developmental abnormalities in hypospadiac male rats induced by maternal exposure to di-n-butyl phthalate (DBP).

Author

Jiang J, Ma L, Yuan L, Wang X, and Zhang W

Subjects

Animals, Animals, Newborn, Birth Weight drug effects, Dose-Response Relationship, Drug, Female, Histocytochemistry, Hypospadias blood, Hypospadias pathology, Litter Size drug effects, Male, Organ Size drug effects, Pregnancy, Random Allocation, Rats, Rats, Sprague-Dawley, Testosterone blood, Dibutyl Phthalate toxicity, Disease Models, Animal, Hypospadias chemically induced, Maternal Exposure

Abstract

The objective of this study was to establish a hypospadiac rat model by maternal exposure to di-n-butyl phthalate (DBP) and to evaluate the developmental abnormalities of hypospadiac male rats. Timed-pregnant rats were given DBP by gastric intubation at doses of 0, 250, 500, 750 or 1000 mg/kg body weight (bw)/day from gestation day (GD) 14 to 18 to establish a hypospadiac rat model. The hypospadias was observed in the 500 and 750 mg/kg bw/day groups, the incidence of which was 6.8 and 41.3%, respectively. Transverse serial histological analysis of genitalia of hypospadiac male rats confirmed the malformation. With exposed dose increasing, the serum testosterone (T) levels of male rats inversely decreased, and in the same dosage group the serum T levels of hypospadiac rats were significantly lower than the levels of nonhypospadiac counterparts. The other reproductive lesions such as cryptorchidism and decreased ratio of anogenital distance/body weight (AGD/bw) were also observed. Autopsy analysis revealed the development of reproductive organs (prostate, testes, epididymis, pituitary gland) and nonreproductive organs (adrenal gland, liver, kidney, heart, spleen) of hypospadiac rats and nonhypospadiac counterparts. The results indicated that the reproductive system and developmental condition of hypospadiac male offspring were damaged severely by DBP.

Published

2007

2. Maternal exposure to Di-n-butyl phthalate (DBP) inhibit orexin receptor 1 (OX1R) expression to prevent Sertoli cells proliferation through the AKT signaling pathway.

Author

Xie, Zhiwen, Jiang, Juntao, Li, Tiewen, Xu, Xinyu, Wu, Lei, Zhang, Yongqing, Chen, Min, and Sun, Yang

Subjects

SERTOLI cells, DIBUTYL phthalate, GENE expression, CELLULAR signal transduction, MATERNAL exposure

Abstract

Background: Studies have demonstrated that Sertoli cells are the direct target of Dibutyl phthalate (DBP). However, the role of neurotransmitter receptors is not elucidated. Methods: Based on our previous studies, maternal Sprague–Dawley (SD) rats in Gestation Day (GD) 14–18 and TM4 cells exposure to 750 mg/kg/day and 100 μM DBP were regarded as treated groups. Firstly, qRT-PCR array was used to determine the different expression of neurotransmitter receptors. We examined the OX1R expression on Rats in Control and DBP groups by immunohistochemistry. Real-time PCR and Western Blot were used to detect the protein and mRNA expression levels of OX1R in vivo and in vitro. The potential downstream signaling pathways were explored by analyzing the GSE99690 cohort. In addition, we extracted Primary Sertoli Cells (PSCs) from the testis of control group. The apoptosis-related proteins, AKT signaling pathway-related proteins and mRNA expressions were detected by Western Blot and Real-time PCR in PSCs. The validity of PSCs was measured by CCK-8 assay and flow cytometric analysis was used to demonstrate the apoptotic rates of PSCs after DBP exposure. Results: The Orexin receptor 1 (OX1R) was screened out by qRT-PCR array. Our results showed that DBP could significantly suppress the OX1R expression of Sertoli cells in vivo and in vitro. Functional analysis showed the AKT signaling pathway was mediated by OX1R. The highly expressed apoptosis level and impaired cell activity were observed in PSCs, which can be reversed by Orexin A. Meanwhile, the p-AKT signaling pathway were hindered after DBP exposure while rescued in DBP + Orexin-A group. Conclusions: DBP can induce Sertoli cell apoptosis through its toxicological effect by suppressing OX1R and p-AKT expression, which provide a novel insight on the role of neurotransmitter receptors. [ABSTRACT FROM AUTHOR]

Published

2024

3. Maternal exposure to dibutyl phthalate (DBP) impairs angiogenesis and AR signalling pathway through suppression of TGFB1I1 in hypospadias offspring.

Author

Wu, Lei, Shi, Fei, Zhang, Yongqing, Xu, Xinyu, Xie, Zhiwen, Hua, Shan, Xia, Shujie, and Jiang, Juntao

Subjects

DIBUTYL phthalate, MATERNAL exposure, TRANSFORMING growth factors-beta, CELLULAR signal transduction, HYPOSPADIAS, NEOVASCULARIZATION, DYSPLASIA

Abstract

Early exposure to dibutyl phthalate (DBP) can cause hypospadias in newborn foetuses. However, the underlying molecular mechanism is not well defined. Aberrant angiogenesis is associated with various dysplasias including urogenital deficits. In vivo and in vitro angiogenesis assays showed reduced angiogenesis in the hypospadias group and DBP exposed group. RNA-sequencing analysis of DBP-treated HUVECs revealed decreased expression of transforming growth factor beta 1-induced transcript 1 (TGFB1I1) and a significantly enriched angiogenesis-associated pathway. Further experiments revealed that decreased TGFB1I1 expression was associated with disrupted tube formation and migration, which resulted in decreased angiogenesis. Functional assays revealed that the overexpression of TGFB1I1 promoted tube formation and migration of HUVECs in the DBP-treated group. Moreover, we showed that the transcription factor AR was regulated by TGFB1I1 through inhibiting its translocation from the cytoplasm to the nucleus. Together, our results identified TGFB1I1 as a component of aberrant angiogenesis in hypospadias rats and its interaction with AR might be a potential target for hypospadias development. [Display omitted] • Maternal exposure to DBP impaired in vivo and in vitro angiogenesis. • Decreased TGFB1I1 was associated with microvessel density in hypospadias. • TGFB1I1 impairs angiogenesis and nucleus translocation of AR after DBP exposure. [ABSTRACT FROM AUTHOR]

Published

2024

4. Prenatal exposure to di-n-butyl phthalate promotes RIPK1-regulated necroptosis of uroepithelial cells and induces hypospadias through the epithelial-mesenchymal transition process in newborn male rats.

Author

Wu, Lei, Xie, Zhiwen, Li, Tiewen, Chen, Xincan, Jiang, Juntao, Shi, Fei, Zhang, Yongqing, Xu, Xinyu, Xia, Shujie, and Sun, Wenlan

Subjects

*ANDROGEN receptors, *EPITHELIAL-mesenchymal transition, *WESTERN immunoblotting, *CORN oil, *MATERNAL exposure, *PROTEOLYSIS

Abstract

Maternal exposure to di-n-butyl phthalate (DBP) has been linked to the induction of hypospadias; however, the underlying mechanism remains unclear. Necroptosis is reported to be implicated in developmental malformations. This study aimed to investigate the underlying mechanism of necroptosis in the development of hypospadias. DBP was dissolved in corn oil, and pregnant rats were administered a precisely measured dose of DBP (750 mg/kg/day) via gastric intubation from gestation day 14–18. Control rats received only corn oil. The day of birth was considered postnatal day (PND) 1. Male hypospadias rats were identified on PND 7. Genital tubercle tissues were collected and stored at −80°C for subsequent PCR analysis, cryopreserved in liquid nitrogen for western blot, or fixed in formalin for immunohistochemistry (IHC) staining. IHC staining and western blot analysis revealed increased expression of RIPK1 and necroptosis markers in genital tubercle (GT) tissue compared to the control group. Additionally, higher levels of EMT and impaired androgen receptor expression were observed in GT tissue. Exposure to increased DBP concentrations in rat primary uroepithelial cells (PUCs) led to elevated ROS production. Necroptosis markers and EMT expression levels were upregulated in PUCs following DBP incubation. Notably, treatment with DBP combined with necrostatin-1, a necroptosis inhibitor, reduced the expression of EMT markers and ROS production compared to DBP treatment alone. In vitro studies further revealed that DBP-induced necroptosis promoted the degradation of E-cadherin through the ubiquitin-proteasome pathway in PUCs. Our findings suggest that maternal exposure to DBP promotes necroptosis in uroepithelial cells by elevating ROS level and EMT status. Thus, necroptosis may play an essential role in the development of hypospadias. [Display omitted] • Maternal exposure to DBP promoted EMT expression in hypospadias offspring. • DBP-induced necroptosis elevated EMT level in hypospadias genital tubercles. • Necroptosis induced E-cadherin degradation via ubiquitin proteasome pathway. [ABSTRACT FROM AUTHOR]

Published

2024