Kbtbd11 gene expression in adipose tissue increases in response to feeding and affects adipocyte differentiation

Biochemistry and Biophysics Reports

Yokota

Yoshida

et al. 2019

Self Cite

N4BP2l1, which is highly expressed in oral squamous cell carcinoma, is associated with poor prognosis. However, N4bp2l1 's role in adipogenesis remains unknown. We aimed to clarify the expression profile and transcriptional regulation of N4bp2l1 to elucidate the functions underlying the role of N4bp2l1 in adipocyte differentiation. Our results revealed that N4bp2l1 mRNA expression increased in 3T3-L1 cells in a differentiation-dependent manner. To investigate the transcriptional regulation of N4bp2l1 , the 2-kb 5′ region upstream of the mouse N4bp2l1 promoter was cloned into a luciferase vector. Luciferase reporter assays indicated that USF1 induces the N4bp2l1 promoter activity. Electrophoretic mobility shift and chromatin immunoprecipitation assays confirmed that USF1 directly binds to the Ebox in the N4bp2l1 promoter. Furthermore, the expressions of adipocyte differentiation markers significantly decreased in N4bp2l1 -knockdown cells compared with those in control cells. Our results demonstrated that N4bp2l1 is a novel USF1 target gene that may be involved in adipogenesis regulation.

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

A novel upstream transcription factor 1 target gene N4bp2l1 that regulates adipogenesis

Biochemistry and Biophysics Reports

Yokota

Yoshida

et al. 2019

Self Cite

“…The BTB/POZ domain functions as the protein–protein interaction domain to facilitate dimer formation and interaction with nonBTB domain comprising proteins, involving activities such as transcriptional regulation, cytoskeleton dynamics, ion channel assembly and gating, and protein ubiquitination/degradation [1]. The Kelch domain, which is widely conserved in mammals and insects, usually comprises 2–7 repeats of four-stranded beta-sheet motifs that form the beta-propeller structure [2]. The Kelch β-propellers primarily function as scaffolds for protein–protein interactions.…”

Section: Introductionmentioning

confidence: 99%

“…We have previously reported that Kbtbd11 is involved in nutritional regulation and is highly expressed in the epididymal white adipose tissue (eWAT) in diet-induced obesity (DIO) mice compared with that in mice fed on chow diet [2]. In addition, the adenovirus-mediated knockdown of Kbtbd11 in 3T3-L1 cells inhibits mitotic clonal expansion (MCE), which is required during the early stages of 3T3-L1 adipocyte differentiation [2]. In contrast, Kbtbd11 -overexpressing 3T3-L1 promotes MCE, which leads to the expression of adipocyte differentiation markers —C/ebpa and Pparg , and induces lipid accumulation [2], suggesting that Kbtbd11 expression levels play a major role in MCE and influence triglyceride accumulation and adipocyte differentiation.…”

Section: Introductionmentioning

confidence: 99%

“…In addition, the adenovirus-mediated knockdown of Kbtbd11 in 3T3-L1 cells inhibits mitotic clonal expansion (MCE), which is required during the early stages of 3T3-L1 adipocyte differentiation [2]. In contrast, Kbtbd11 -overexpressing 3T3-L1 promotes MCE, which leads to the expression of adipocyte differentiation markers —C/ebpa and Pparg , and induces lipid accumulation [2], suggesting that Kbtbd11 expression levels play a major role in MCE and influence triglyceride accumulation and adipocyte differentiation. In this context, the present study aimed to clarify the transcriptional regulation of Kbtbd11 to elucidate the functions underlying the role of Kbtbd11 in adipocyte differentiation.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Kbtbd11 contributes to adipocyte homeostasis through the activation of upstream stimulatory factor 1

Yokota

Yoshida

et al. 2019

Heliyon

Self Cite

The present study aimed to investigate the transcriptional regulation of Kbtbd11 in adipose tissue. To elucidate the physiological role of Kbtbd11 gene expression, adipose Kbtbd11 mRNA expression levels were estimated under various feeding states in wild-type mice. Kbtbd11 expression increased in a time-dependent manner in the adipose tissue in mice fed on chow diet, whereas the promotion of Kbtbd11 mRNA expression by refeeding was attenuated in mice fed on high-fat (HF) diet, suggesting the suppression of Kbtbd11 mRNA expression under HF diets and that changes in mRNA levels were associated with regulation of the transcription activity of Kbtbd11 by some transcription factors. To investigate the transcriptional regulation of Kbtbd11, the fragment upstream of either mouse Kbtbd11 or human KBTBD11 promoter was inserted into a luciferase vector. Luciferase reporter assays revealed that both mouse and human KBTBD11 promoter activity was increased by USF1. Direct USF1 binding to the Ebox in the Kbtbd11 promoter was confirmed by electrophoretic mobility shift and chromatin immunoprecipitation assays. In addition, the adipocyte differentiation marker levels increased instantly in Kbtbd11-overexpressing Usf1 knockdown cells than in Usf1 knockdown cells. These results imply an association of between Kbtbd11 with Usf1 expression and suggest the involvement of Kbtbd11 in a novel adipogenesis pathway.

ILDR2 stabilization is regulated by its interaction with GRP78

Nakayama

Ohta

et al. 2021

Sci Rep

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Ildr2 was initially identified as a genetic modifier of diabetes susceptibility in B6.DBA Lepob congenic mice, and was associated with decreased β-cell replication rates, reduced β-cell mass, and persistent mild hypoinsulinemic hyperglycemia. However, the molecular mechanisms of how the ILDR2 protein is involved in these effects are largely unknown. We sought to identify ILDR2-interacting proteins to further elucidate the molecular mechanisms underpinning ILDR2 function in pancreatic β-cells. Using TAP tag technology, we purified proteins interacting with ILDR2 in the pancreatic β-cell line MIN6, and identified the endoplasmic reticulum resident chaperones, GRP78 and PDIA1, as novel proteins interacting with ILDR2. We demonstrated that GRP78 interacted with ILDR2 and was possibly involved in ILDR2 stabilization by inhibiting ubiquitin–proteasome degradation. Additionally, adenoviral ILDR2 knockdown led to reduced glucose-responsive insulin secretion in MIN6 β-cells, suggesting ILDR2 may be implicated in a new pathway in hypoinsulinemic hyperglycemia. These data provide evidence for a novel association between GRP78 and ILDR2, and suggest GPR78-ILDR2 may a novel target for diabetic therapeutic modulation in decreased insulin secretion.