Lack of bombesin receptor–activated protein attenuates bleomycin-induced pulmonary fibrosis in mice

Wang, Hui; Zhang, Wenrui; Liu, Rujiao; Zheng, Jiaoyun; Yao, Xueping; Chen, Hui; Wang, Jie; Weber, H. Christian; Qin, Xiaoqun; Xiang, Yang; Liu, Chi; Liu, Huijun; Pan, Lang; Qu, Xiangping

doi:10.26508/lsa.202201368

Cited by 6 publications

(23 citation statements)

References 41 publications

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“…1, BRAP was present in bronchial epithelial cells within lung tissue samples from patients with interstitial lung disease, pulmonary tuberculosis, pulmonary fibrosis, and lung squamous cell carcinoma. We have generated BC004004 −/− mice using CRISPR/Cas9‐mediated genome engineering method to investigate the role of BRAP homologous protein as described previously [11]. The trachea tissues were isolated from BC004004 −/− mice and their isogenic wild‐type control BC004004 +/+ mice in order to examine whether BRAP homolog was involved in maintaining the morphology of airway cilia.…”

Section: Resultsmentioning

confidence: 99%

“…Total RNA was extracted from lung tissues or isolated cells using RNAiso Plus (Takara, Beijing, China, cat: 9108) according to the manufacturer's instructions as described previously [11]. Next, 1.0 lg of total RNA was reversely transcribed into complementary DNA (cDNA) using the Prime Script TM RT reagent Kit with gDNA Eraser (Takara, cat: RR047B), and quantitative real-time PCR analyses were conducted using SYBRÒ Premix Ex Taq TM II system (Takara, cat: RR420A) on a deep well Real-Time PCR Detection System (CFX96 Touch TM ; Bio-Rad, Hercules, CA, USA) as described previously [11]. Each sample was analyzed in triplicate.…”

Section: Gene Expression Analysis By Quantitative Realtime Reverse-tr...mentioning

confidence: 99%

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Knockout of the BRAP homolog in mice leads to abnormal tracheal cilia

Wang,

Zuo,

Zheng

et al. 2023

FEBS Letters

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Both bombesin receptor‐activated protein (BRAP) and its mouse homolog have been found to be expressed in bronchial epithelia but with unclear functions. Using electron microscopy combined with histological assays, we found that BRAP homolog deficiency in mice led to abnormal tracheal cilia. Rab‐3A‐interacting protein (Rabin8), a protein that might play a role in cilia development, was screened by yeast two‐hybrid and further verified to have interaction with human BRAP by co‐immunoprecipitation and pull down assays. The expression levels of Rabin 8, together with acetylated α‐tubulin, a marker of cilia, were either downregulated by knockdown of BRAP or upregulated by overexpression of BRAP in cultured immortalized human bronchial epithelial cells. These results reveal a role for BRAP in airway cilia formation.

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Section: Resultsmentioning

confidence: 99%

Section: Gene Expression Analysis By Quantitative Realtime Reverse-tr...mentioning

confidence: 99%

Knockout of the BRAP homolog in mice leads to abnormal tracheal cilia

Wang,

Zuo,

Zheng

et al. 2023

FEBS Letters

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“…All clinical samples were obtained from the department of pathology at the second xiangya hospital, and human experiments were conducted in accordance with the standard operating guidelines of the Institutional Animal Care and Research Advisory Committee of Central South University, Changsha, China (No: 2022-KT118). Seven weeks old female BC004004 -/- mice, in which BC004004 gene was disrupted by CRISPR/Cas9-mediated genome engineering technique 12 , and their isogenic control C57BL/6 mice ( BC004004 +/+ ) were used in the study.…”

Section: Methodsmentioning

confidence: 99%

“…The mouse homolog of BRAP, which is encoded by BC004004 gene and shares 83% similarity to the human BRAP, was also expressed in mouse skin. In our previous study, we investigated the function of BRAP and its mouse homolog by utilizing a gene knockout mouse model BC004004 -/- , which led to several distinct phenotypes 12 - 14 . Compared with their isogenic wild type control, BC004004 -/- mice exhibited attenuation of injury induced fibrosis in both lungs 12 and kidneys (data not published), exacerbation of stress induced behavioral changes 13 and abnormal cilia formation in trachea epithelial cells 14 .…”

Section: Introductionmentioning

confidence: 99%

“…In our previous study, we investigated the function of BRAP and its mouse homolog by utilizing a gene knockout mouse model BC004004 -/- , which led to several distinct phenotypes 12 - 14 . Compared with their isogenic wild type control, BC004004 -/- mice exhibited attenuation of injury induced fibrosis in both lungs 12 and kidneys (data not published), exacerbation of stress induced behavioral changes 13 and abnormal cilia formation in trachea epithelial cells 14 . The underlying cellular and molecular mechanisms remain largely unknown, but our studies provide evidence for altered behaviors of several cell types including lung fibroblasts, tubular epithelial cells and neurons due to lack of BRAP expression.…”

Section: Introductionmentioning

confidence: 99%

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Bombesin receptor-activated protein homolog deficiency altered the pattern of pathological changes of psoriasis - like skin lesion in mice

Zheng,

Wang,

Wang

et al. 2024

Int. J. Med. Sci.

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This study investigated the potential role of the mouse homolog of bombesin receptor-activated protein (BRAP) in imiquimod (IMQ) induced psoriasis - like skin inflammation. The expression of both human BRAP, encoded by C6orf89 , and its mouse homolog, encoded by BC004004 , has been found to be expressed abundantly in the keratinocytes. BC004004 knockout mice ( BC004004 -/- ) were topically treated with IMQ daily for 7 days to test whether they were more vulnerable to psoriasis - like inflammation. We found that those mice exhibited an altered pattern of inflammation process compared to isogenic wild type control mice ( BC004004 +/+ ). BC004004 -/- mice developed skin lesions with earlier and more acute onset, as well as a quicker remission. The cytokines related to pathogenesis of psoriasis also exhibited different expression patterns in IMQ treated BC004004 -/- mice. On day 4 of IMQ treatment, BC004004 -/- mice exhibited a higher expression level of IL-17A compared to BC004004 +/+ mice, suggesting a more robust activation of Th17 cells in the knockout mice. The serum level of thymic stromal lymphopoietin (TSLP), one of the keratinocyte derived cytokines, was also increased in BC004004 -/- mice and reached its peak on day 4. Knockdown of BRAP in cultured human keratinocyte-derived HaCaT cells by siRNA silencing led to increased release of TSLP. Our data suggest that the elevated of level of TSLP released from keratinocytes due to BRAP deficiency might mediate the crosstalk between the epidermal cells and immune cells and thereby contributing to the altered pathological changes observed in psoriasis - like skin lesion in knockout mice.

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