Your search keyword '"FHL1"' showing total 395 results

1. FHL1: A novel diagnostic marker for papillary thyroid carcinoma.

Author

Zeng, Yeting, Zeng, Dehua, Qi, Xingfeng, Wang, Hanxi, Wang, Xuzhou, Dai, Xiaodong, and Qu, Lijuan

Subjects

*IMMUNOSTAINING, *GENE expression, *POLYMERASE chain reaction, *PAPILLARY carcinoma, *TUMOR markers

Abstract

Although there are clear morphologic criteria for the diagnosis of papillary thyroid carcinoma (PTC), when the morphology is untypical or overlaps, accurate diagnostic indicators are necessary. Since few studies investigated the role of down‐regulated genes in PTC, this article aims to further explore the molecular markers associated with PTC. We conducted bioinformatics analysis of gene microarrays of PTC and normal adjacent tissues. Besides, quantitative real‐time quantitative polymerase chain reaction array and immunohistochemical staining were used to investigate the expression of the major down‐regulated genes. The results indicated that several important down‐regulated genes, including TLE1, BCL2, FHL1, GHR, KIT, and PPARGC1A were involved in the process of PTC. Compared to normal adjacent tissues, the mRNA expression of the major genes was down‐regulated in PTC (p＜0.05). Immunohistochemically, FHL1 shows negative or low expression in PTC tissues (p＜0.05). BCL2 did not show a significant difference between PTC and normal thyroid tissues (p > 0.05). TLE1, KIT, PPARGC1A and GHR showed negative expression in both tumor and normal tissues. These results suggested that FHL1 could serve as a novel tumor marker for precise diagnosis of PTC. [ABSTRACT FROM AUTHOR]

Published

2024

2. MiR-223-3p Promotes Osteoporosis Progression by Repressing Osteogenic Differentiation via Targeting FHL1/Wnt/β-catenin Signaling

Author

Shi, Kairi, Wei, Junyu, and Chen, Jianming

Published

2024

3. Long non-coding RNA Small Nucleolar RNA Host Gene 4 ameliorates cigarette smoke-induced proliferation, apoptosis, inflammation, and airway remodeling in alveolar epithelial cells through the modulation of the mitogen-activated protein kinase signaling pathway via the microRNA-409-3p/Four and a Half LIM Domains 1 axis

Author

Meng Liu, JiGuang Meng, XuXin Chen, Fan Wang, and ZhiHai Han

Subjects

Lnc SNHG4, miR-409-3p, FHL1, MAPK, COPD, Medicine

Abstract

Abstract The long non-coding RNA (lncRNA) Small Nucleolar RNA Host Gene 4 (SNHG4) has been demonstrated to be significantly downregulated in various inflammatory conditions, yet its role in chronic obstructive pulmonary disease (COPD) remains elusive. This study aims to elucidate the biological function of SNHG4 in COPD and to unveil its potential molecular targets. Our findings reveal that both SNHG4 and Four and a Half LIM Domains 1 (FHL1) were markedly downregulated in COPD, whereas microRNA-409-3p (miR-409-3p) was upregulated. Importantly, SNHG4 exhibited a negative correlation with inflammatory markers in patients with COPD, but a positive correlation with forced expiratory volume in 1s percentage (FEV1%). SNHG4 distinguished COPD patients from non-smokers with high sensitivity, specificity, and accuracy. Overexpression of SNHG4 ameliorated cigarette smoke extract (CSE)-mediated inflammation, apoptosis, oxidative stress, and airway remodeling in 16HBE bronchial epithelial cells. These beneficial effects of SNHG4 overexpression were reversed by the overexpression of miR-409-3p or the silencing of FHL1. Mechanistically, SNHG4 competitively bound to miR-409-3p, mediating the expression of FHL1, and consequently improving inflammation, apoptosis, oxidative stress, and airway remodeling in 16HBE cells. Additionally, SNHG4 regulated the miR-409-3p/FHL1 axis to inhibit the activation of the mitogen-activated protein kinase (MAPK) pathway induced by CSE. In a murine model of COPD, knockdown of SNHG4 exacerbated CSE-induced pulmonary inflammation, apoptosis, and oxidative stress. In summary, our data affirm that SNHG4 mitigates pulmonary inflammation, apoptosis, and oxidative damage mediated by COPD through the regulation of the miR-409-3p/FHL1 axis. Graphical Abstract

Published

2024

4. Long non-coding RNA Small Nucleolar RNA Host Gene 4 ameliorates cigarette smoke-induced proliferation, apoptosis, inflammation, and airway remodeling in alveolar epithelial cells through the modulation of the mitogen-activated protein kinase signaling pathway via the microRNA-409-3p/Four and a Half LIM Domains 1 axis

Author

Liu, Meng, Meng, JiGuang, Chen, XuXin, Wang, Fan, and Han, ZhiHai

Abstract

The long non-coding RNA (lncRNA) Small Nucleolar RNA Host Gene 4 (SNHG4) has been demonstrated to be significantly downregulated in various inflammatory conditions, yet its role in chronic obstructive pulmonary disease (COPD) remains elusive. This study aims to elucidate the biological function of SNHG4 in COPD and to unveil its potential molecular targets. Our findings reveal that both SNHG4 and Four and a Half LIM Domains 1 (FHL1) were markedly downregulated in COPD, whereas microRNA-409-3p (miR-409-3p) was upregulated. Importantly, SNHG4 exhibited a negative correlation with inflammatory markers in patients with COPD, but a positive correlation with forced expiratory volume in 1s percentage (FEV1%). SNHG4 distinguished COPD patients from non-smokers with high sensitivity, specificity, and accuracy. Overexpression of SNHG4 ameliorated cigarette smoke extract (CSE)-mediated inflammation, apoptosis, oxidative stress, and airway remodeling in 16HBE bronchial epithelial cells. These beneficial effects of SNHG4 overexpression were reversed by the overexpression of miR-409-3p or the silencing of FHL1. Mechanistically, SNHG4 competitively bound to miR-409-3p, mediating the expression of FHL1, and consequently improving inflammation, apoptosis, oxidative stress, and airway remodeling in 16HBE cells. Additionally, SNHG4 regulated the miR-409-3p/FHL1 axis to inhibit the activation of the mitogen-activated protein kinase (MAPK) pathway induced by CSE. In a murine model of COPD, knockdown of SNHG4 exacerbated CSE-induced pulmonary inflammation, apoptosis, and oxidative stress. In summary, our data affirm that SNHG4 mitigates pulmonary inflammation, apoptosis, and oxidative damage mediated by COPD through the regulation of the miR-409-3p/FHL1 axis. Highlights: SNHG4 and FHL1 were aberrantly downregulated in COPD, while miR-409-3p was upregulated. Overexpression of SNHG4 mitigated CSE-mediated inflammation, apoptosis, and oxidative stress in 16HBE cells. The salutary effects of SNHG4 overexpression in 16HBE cells were reversed upon overexpression of miR-409-3p or silencing of FHL1. SNHG4 competitively bound miR-409-3p to modulate FHL1 expression. Through the miR-409-3p/FHL1 axis, SNHG4 inhibited the activation of the MAPK signaling pathway in the context of COPD. [ABSTRACT FROM AUTHOR]

Published

2024

5. Low FHL1 expression indicates a good prognosis and drug sensitivity in ovarian cancer.

Author

Chen, Xiaoying, Yu, Yue, Su, Yuting, Shi, Lizhou, Xie, Shanzhou, Hong, Yi, Liu, Xia, and Yin, Fuqiang

Abstract

Chemotherapy resistance is the main reason for the poor prognosis of ovarian cancer (OC). FHL1 is an important tumour regulator, but its relationship with the prognosis, drug resistance, and tumour microenvironment of OC is unknown. Immunohistochemistry was used to determine FHL1 expression in OC. Kaplan‒Meier plotter was used for survival analysis. The value of gene expression in predicting drug resistance was estimated using the area under the curve (AUC). Bivariate correlation was used to determine the coexpression of two genes. Functional cluster and pathway enrichment were used to uncover hidden signalling pathways. The relationship between gene levels and the tumour microenvironment was visualised through the ggstatsplot and pheatmap packages. The mRNA and protein levels of FHL1 were downregulated in 426 and 100 OC tissues, respectively. Low FHL1 expression was correlated with good progression-free survival (PFS), postprogression survival, and overall survival (OS) in 1815 OC patients, and was further confirmed to be associated with good OS by immunohistochemistry in 152 OC tissues. Furthermore, FHL1 was downregulated in drug-sensitive tissues, while its high expression predicted drug resistance (AUC > 0.65). Mechanistically, FHL1 was coexpressed with FLNC, CAV1, PPP1R12B, and FLNA at the mRNA and protein levels in 558 and 174 OC tissues, respectively, and their expression was downregulated in OC. Additionally, very strong coexpression of FHL1 with the four genes was identified in at least 23 different tumours. Low expression of the four genes was associated with good PFS, and the combination of FHL1 with the four genes provided better prognostic power. Meanwhile, the expression of all five genes was strongly and positively associated with the abundance of macrophages. Low FHL1 expression acts as a favourable factor in OC, probably via positive coexpression with FLNC, CAV1, PPP1R12B, and FLNA. [ABSTRACT FROM AUTHOR]

Published

2024

6. Global comparative transcriptomes uncover novel and population-specific gene expression in esophageal squamous cell carcinoma

Author

Amal Alotaibi, Veerendra P. Gadekar, Pranav Swaroop Gundla, Sumana Mandarthi, Nidhi Jayendra, Asna Tungekar, B. V. Lavanya, Ashok Kumar Bhagavath, Mary Anne Wong Cordero, Janne Pitkaniemi, Shaik Kalimulla Niazi, Raghavendra Upadhya, Asmatanzeem Bepari, and Prashantha Hebbar

Subjects

Novel genes in ESCC, CHRM3, CREG2, H2AC6, ENDOU, FHL1, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Esophageal squamous cell carcinoma (ESCC) has a poor prognosis and is one of the deadliest gastrointestinal malignancies. Despite numerous transcriptomics studies to understand its molecular basis, the impact of population-specific differences on this disease remains unexplored. Aims This study aimed to investigate the population-specific differences in gene expression patterns among ESCC samples obtained from six distinct global populations, identify differentially expressed genes (DEGs) and their associated pathways, and identify potential biomarkers for ESCC diagnosis and prognosis. In addition, this study deciphers population specific microbial and chemical risk factors in ESCC. Methods We compared the gene expression patterns of ESCC samples from six different global populations by analyzing microarray datasets. To identify DEGs, we conducted stringent quality control and employed linear modeling. We cross-compared the resulting DEG lists of each populations along with ESCC ATLAS to identify known and novel DEGs. We performed a survival analysis using The Cancer Genome Atlas Program (TCGA) data to identify potential biomarkers for ESCC diagnosis and prognosis among the novel DEGs. Finally, we performed comparative functional enrichment and toxicogenomic analysis. Results Here we report 19 genes with distinct expression patterns among populations, indicating population-specific variations in ESCC. Additionally, we discovered 166 novel DEGs, such as ENDOU, SLCO1B3, KCNS3, IFI35, among others. The survival analysis identified three novel genes (CHRM3, CREG2, H2AC6) critical for ESCC survival. Notably, our findings showed that ECM-related gene ontology terms and pathways were significantly enriched among the DEGs in ESCC. We also found population-specific variations in immune response and microbial infection-related pathways which included genes enriched for HPV, Ameobiosis, Leishmaniosis, and Human Cytomegaloviruses. Our toxicogenomic analysis identified tobacco smoking as the primary risk factor and cisplatin as the main drug chemical interacting with the maximum number of DEGs across populations. Conclusion This study provides new insights into population-specific differences in gene expression patterns and their associated pathways in ESCC. Our findings suggest that changes in extracellular matrix (ECM) organization may be crucial to the development and progression of this cancer, and that environmental and genetic factors play important roles in the disease. The novel DEGs identified may serve as potential biomarkers for diagnosis, prognosis and treatment.

Published

2023

7. Anti-oncogenic mechanism of KLF17 in colon cancer by repressing cell migration and invasion via FHL1 upregulation.

Author

Yi, Shengen, Luo, Ming, Peng, Yanjin, Chen, Yong, and Yu, Dan

Subjects

COLON cancer, CANCER cell migration, KRUPPEL-like factors, PROTEIN domains, POLYMERASE chain reaction

Abstract

Colon cancer is a disease with high prevalence worldwide. This study sought to investigate Kruppel-like factor 17 (KLF17) mechanism in the development of colon cancer through four-and-a-half-LIM domain protein 1 (FHL1). In colon cancer cells, KLF17 and FHL1 expression was detected by reverse transcription-quantitative polymerase chain reaction (RT-qPCR) and Western blot. After gain- and loss-of-function experiments in colon cancer cells, cell proliferative, invasive, and migrating abilities were tested by cell counting kit-8, transwell, and scratch assays, respectively. The expression of epithelial–mesenchymal transition (EMT)-related genes, E-cadherin, N-cadherin, and Vimentin, was measured by RT-qPCR and Western blot. Chromatin immunoprecipitation and dual-luciferase reporter gene assays were performed to detect the binding of KLF17 and the FHL1 promoter. Finally, a transplantation tumor model in nude mice was established for in vivo validation. Mechanistically, KLF17 facilitated FHL1 transcription by binding to the FHL1 promoter. KLF17 or FHL1 upregulation suppressed the colon cancer cell proliferative, invasive, and migrating capacities, accompanied by elevated E-cadherin expression and diminished N-cadherin and Vimentin expression. Furthermore, FHL1 silencing abrogated the repressive impacts of KLF17 upregulation on colon cancer cell EMT, proliferative, invasive, and migrating capabilities. Furthermore, KLF17 augmented FHL1 expression and curtailed the growth of transplanted tumors in nude mice. Conclusively, KLF17 promoted FHL1 transcription, thereby impeding the invasion, migration, and EMT of colon cancer cells. [ABSTRACT FROM AUTHOR]

Published

2023

8. Global comparative transcriptomes uncover novel and population-specific gene expression in esophageal squamous cell carcinoma.

Author

Alotaibi, Amal, Gadekar, Veerendra P., Gundla, Pranav Swaroop, Mandarthi, Sumana, Jayendra, Nidhi, Tungekar, Asna, Lavanya, B. V., Bhagavath, Ashok Kumar, Cordero, Mary Anne Wong, Pitkaniemi, Janne, Niazi, Shaik Kalimulla, Upadhya, Raghavendra, Bepari, Asmatanzeem, and Hebbar, Prashantha

Subjects

*DIAGNOSIS of esophageal cancer, *ESOPHAGEAL cancer risk factors, *META-analysis, *MICROARRAY technology, *RISK assessment, *GENE expression profiling, *SURVIVAL analysis (Biometry), *GENOMICS, *RESEARCH funding, *TUMOR markers, *TOXICOLOGY, *SQUAMOUS cell carcinoma, *ESOPHAGEAL cancer

Abstract

Background: Esophageal squamous cell carcinoma (ESCC) has a poor prognosis and is one of the deadliest gastrointestinal malignancies. Despite numerous transcriptomics studies to understand its molecular basis, the impact of population-specific differences on this disease remains unexplored. Aims: This study aimed to investigate the population-specific differences in gene expression patterns among ESCC samples obtained from six distinct global populations, identify differentially expressed genes (DEGs) and their associated pathways, and identify potential biomarkers for ESCC diagnosis and prognosis. In addition, this study deciphers population specific microbial and chemical risk factors in ESCC. Methods: We compared the gene expression patterns of ESCC samples from six different global populations by analyzing microarray datasets. To identify DEGs, we conducted stringent quality control and employed linear modeling. We cross-compared the resulting DEG lists of each populations along with ESCC ATLAS to identify known and novel DEGs. We performed a survival analysis using The Cancer Genome Atlas Program (TCGA) data to identify potential biomarkers for ESCC diagnosis and prognosis among the novel DEGs. Finally, we performed comparative functional enrichment and toxicogenomic analysis. Results: Here we report 19 genes with distinct expression patterns among populations, indicating population-specific variations in ESCC. Additionally, we discovered 166 novel DEGs, such as ENDOU, SLCO1B3, KCNS3, IFI35, among others. The survival analysis identified three novel genes (CHRM3, CREG2, H2AC6) critical for ESCC survival. Notably, our findings showed that ECM-related gene ontology terms and pathways were significantly enriched among the DEGs in ESCC. We also found population-specific variations in immune response and microbial infection-related pathways which included genes enriched for HPV, Ameobiosis, Leishmaniosis, and Human Cytomegaloviruses. Our toxicogenomic analysis identified tobacco smoking as the primary risk factor and cisplatin as the main drug chemical interacting with the maximum number of DEGs across populations. Conclusion: This study provides new insights into population-specific differences in gene expression patterns and their associated pathways in ESCC. Our findings suggest that changes in extracellular matrix (ECM) organization may be crucial to the development and progression of this cancer, and that environmental and genetic factors play important roles in the disease. The novel DEGs identified may serve as potential biomarkers for diagnosis, prognosis and treatment. [ABSTRACT FROM AUTHOR]

Published

2023

9. VE-822 upregulates the deubiquitinase OTUD1 to stabilize FHL1 to inhibit the progression of lung adenocarcinoma.

Author

Zhang, Qi, Li, Jinglei, Chen, Zihan, Jiang, Ke, Yang, Kunyu, Huang, Fang, Huang, Ai, Zhang, Xiaodong, Zhang, Jinxiang, and Wang, Hui

Subjects

*CANCER cell migration, *LUNGS, *ADENOCARCINOMA, *LUNG tumors, *LUNG cancer

Abstract

Background: The deubiquitinase ovarian tumor domain-containing 1 (OTUD1) has been considered as a tumor suppressor in many tumors, but there is minimal research on the role of OTUD1 in lung adenocarcinoma (LUAD) pathogenesis. Methods: Bioinformatics analyses and western blot were applied for investigating OTUD1 expression in lung cancer and the drug that upregulated OTUD1. Kaplan–Meier analysis with log-rank test was used for survival analyses. IP-MS and co-IP were performed for identifying potential protein interactions with OTUD1. In vitro and in vivo assays were used for exploring the function of OTUD1 during the progression of LUAD. Results: OTUD1 was dramatically downregulated in tumors and cell lines of human lung cancer. OTUD1 inhibited proliferation and migration of lung cancer cells in vitro. Moreover, OTUD1 inhibited growth of xenografts in nude mice and formation of primary lung tumors in urethane-induced lung cancer model. Mechanistically, we showed that OTUD1 deubiquitinated and stabilized FHL1. Furthermore, we listed and identified VE-822 as a candidate agonist for OTUD1. VE-822 inhibited proliferation of lung adenocarcinoma both in vitro and in vivo. Conclusion: These results indicated that the deubiquitinase OTUD1, which was upregulated by VE-822, inhibited the progression of LUAD in vitro and in vivo by deubiquitinating and stabilizing FHL1. [ABSTRACT FROM AUTHOR]

Published

2023

10. Anti-oncogenic mechanism of KLF17 in colon cancer by repressing cell migration and invasion via FHL1 upregulation

Author

Shengen Yi, Ming Luo, Yanjin Peng, Yong Chen, and Dan Yu

Subjects

colon cancer, fhl1, invasion, kruppel-like factor 17, migration, transcription factor, Physiology, QP1-981

Abstract

Colon cancer is a disease with high prevalence worldwide. This study sought to investigate Kruppel-like factor 17 (KLF17) mechanism in the development of colon cancer through four-and-a-half-LIM domain protein 1 (FHL1). In colon cancer cells, KLF17 and FHL1 expression was detected by reverse transcription-quantitative polymerase chain reaction (RT-qPCR) and Western blot. After gain- and loss-of-function experiments in colon cancer cells, cell proliferative, invasive, and migrating abilities were tested by cell counting kit-8, transwell, and scratch assays, respectively. The expression of epithelial–mesenchymal transition (EMT)-related genes, E-cadherin, N-cadherin, and Vimentin, was measured by RT-qPCR and Western blot. Chromatin immunoprecipitation and dual-luciferase reporter gene assays were performed to detect the binding of KLF17 and the FHL1 promoter. Finally, a transplantation tumor model in nude mice was established for in vivo validation. Mechanistically, KLF17 facilitated FHL1 transcription by binding to the FHL1 promoter. KLF17 or FHL1 upregulation suppressed the colon cancer cell proliferative, invasive, and migrating capacities, accompanied by elevated E-cadherin expression and diminished N-cadherin and Vimentin expression. Furthermore, FHL1 silencing abrogated the repressive impacts of KLF17 upregulation on colon cancer cell EMT, proliferative, invasive, and migrating capabilities. Furthermore, KLF17 augmented FHL1 expression and curtailed the growth of transplanted tumors in nude mice. Conclusively, KLF17 promoted FHL1 transcription, thereby impeding the invasion, migration, and EMT of colon cancer cells.

Published

2023

11. FHL1 Overexpression as A Inhibitor of Lung Cancer Cell Invasion via Increasing RhoGDIß mRNA Expression

Author

Min-ke Shi, Yu-long Xuan, and Xiao-feng He

Subjects

fhl1, invasion, gene expression, lung cancer, rho gdp-dissociation inhibitor beta, Medicine, Science

Abstract

Objective: Four and a half Lin-11, Isl-1, Mac-3 (LIM) protein 1 (FHL1) is one of the FHL protein family, which is regarded as a tumor suppressor in the multiple malignant tumors. In this study, we aimed to explore the regulatory effects and mechanisms of FHL1 on lung cancer cell invasion.Materials and Methods: In this experimental study, bioinformatics analysis of FHL1 transcripts in human lungadenocarcinomas of TCGA database was performed. Quantitative real-time polymerase chain reaction (PCR) was performed to detect FHL1 mRNA expression in 15 paired human lung cancer tissues and their adjacent normal lung tissues, or lung cancer cell lines (A549 and H1299) in comparison with human bronchial epithelial cell line (Beas- 2B). Moreover, western blot was used to analyze FHL1 and rho GDP-dissociation inhibitor beta (RhoGDIβ) protein expression in the indicated cell lines. Also, transwell assays were employed to measure the migrated, and invaded of indicated cell lines.Results: FHL1 transcripts were downregulated in the human lung adenocarcinoma. The impaired FHL1 transcripts were positively correlated with advanced tumor node metastasis (TNM) stage. Moreover, as compared to the adjacent normal lung tissues, FHL1 mRNA was low expressed in 15 paired human lung cancer tissues than their adjacent normal lung tissues. Besides, FHL1 mRNA and protein expression were also reduced in H1299 and A549 cell lines in comparison with Beas-2B cell line. Overexpressed FHL1 protein inhibited the invasive ability of H1299 and A549 cell lines. Mechanically, FHL1 protein overexpression increased the RhoGDIβ protein and mRNA abundance, while knockdown of RhoGDIβ protein, completely restored the invasion ability of A549 (Flag-FHL1) cell line.Conclusion: Our findings indicated that as a key FHL1 downstream regulator, RhoGDIβ is in charge of FHL1 inhibiting lung cancer cell invasion abilities, providing a critical insight into understanding the role of FHL1 for lung cancer development.

Published

2022

12. The role of host factors MXRA8 and FHL1 in arthritogenic alphavirus disease

Author

Ng, Wern Hann and Ng, Wern Hann

Abstract

Arthritogenic alphaviruses, including Chikungunya virus (CHIKV), Ross River virus (RRV), Barmah Forest virus (BFV), Mayaro virus (MAYV), and O'nyong'nyong virus (ONNV), are responsible for debilitating musculoskeletal diseases such as arthralgia, arthritis, and myalgia. These conditions often persist chronically, significantly impairing affected individuals for months or years. Alphaviruses are recognised as emerging pathogens, with their incidence on the rise as they spread to new host populations. Alphaviruses such as RRV and BFV, are endemic to Australia and the Southern Pacific islands, with around 5,000 reported RRV and 1,000 reported BFV cases in Australia annually. In contrast, CHIKV has a global distribution, with cases reported in more than 110 countries across Asia, Africa, Europe, and the Americas since 2005. Notable outbreaks include over 200,000 cases on La Reunion island in 2006, an estimated of about 1.3 million cases in India between 2005-2006, over 2 million cases in the Americas from 2013-2016, around 15,000 cases in Thailand between 2018-2019, and around 80,000 cases in Paraguay between 2022-2023. CHIKV has been identified as a virus to cause the next pandemic. The global impact of CHIKV infection is estimated at over 106,000 disability-adjusted life years (DALYs) annually, making it one of the World Health Organization's top priority Emerging Infectious Diseases and ranking fourth in public health need according to the Coalition for Epidemic Preparedness Innovations. Despite posing a significant public health threat, there is currently no licensed vaccine or available therapy for arthritogenic alphavirus diseases. Understanding host factors is crucial for developing therapeutic strategies. Researchers have made substantial progress in identifying and studying various host factors that play pivotal roles in alphavirus pathogenesis. Although many of these factors have been extensively characterised,knowledge gaps persist, particularly regarding MXR, Thesis (PhD Doctorate), Doctor of Philosophy, School of Pharmacy & Med Sci, Griffith Health, Full Text

Published

2024

13. FHL1 Inhibition by Mir-1301-3p Promotes Uterine Corpus Endometrial Carcinoma Cell Proliferation and Migration: A Prognostic Insight.

Author

Zhu M, Chen B, Miao L, Sun J, Li Y, Zhang P, and Lu X

Abstract

Background: The impact of microRNA-1301-3p (miR-1301-3p) on various cancer subtypes is noteworthy. However, its specific role within the framework of uterine corpus endometrial carcinoma (UCEC) is yet to be clearly defined., Objective: The objective of this research was to investigate and clarify the function of miR-1301-3p in relation to UCEC., Methods: Sample data for our study were sourced from The Cancer Genome Atlas (TCGA). Using various statistical techniques, we assessed the potential of miR-1301-3p as a diagnostic and prognostic indicator, as well as its association with clinical characteristics. Additionally, we conducted an analysis of the genes targeted by miR-1301-3p. The expression levels of miR-1301-3p in uterine corpus endometrial carcinoma (UCEC) cell lines were determined by quantitative real-time PCR (qRT-PCR). Cellular viability and migratory capacity were measured using the CCK8 assay and Transwell migration assays, respectively. Moreover, the expression levels of genes and proteins targeted by miR-1301-3p were identified through dual-luciferase reporter gene assays and Western blot analysis., Results: Expression patterns of miR-1301-3p varied across cancer subtypes, which were significantly linked to specific histological classifications, achieving statistical significance (p < 0.001). In UCEC, higher miR-1301-3p levels correlated with reduced overall survival (p = 0.012) and progression-free survival (p = 0.016), and it emerged as an independent prognostic marker for UCEC. A comparative analysis revealed significantly higher miR-1301-3p levels in UCEC cell lines compared to normal endometrial epithelial cells. Four and a half LIM domains 1 (FHL1) exhibited a negative correlation with miR-1301-3p levels within UCEC tissue samples. miR-1301-3p was shown to promote UCEC cell proliferation and migration through its binding to the 3'-untranslated region (UTR) of the FHL1 gene, thereby repressing FHL1 expression. Additionally, augmenting FHL1 levels was observed to counteract the enhancing impact of miR-1301-3p on UCEC cells., Conclusion: miR-1301-3p regulates the proliferation and migration of UCEC cells by interacting with the FHL1 gene. miR-1301-3p may serve as a promising prognostic biomarker in UCEC., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2024

14. Fhl1, a new spatially specific protein, regulates vein graft neointimal hyperplasia.

Author

Wang C, Chen J, Feng Z, Jian B, Huang S, Feng K, Liu H, Zhou Z, Ye Z, Lu J, Liang M, and Wu Z

Subjects

Animals, Rats, Humans, Male, Disease Models, Animal, Jugular Veins transplantation, Jugular Veins metabolism, Neointima metabolism, Neointima pathology, Neointima genetics, Rats, Sprague-Dawley, Hyperplasia metabolism, Hyperplasia pathology, LIM Domain Proteins genetics, LIM Domain Proteins metabolism, Intracellular Signaling Peptides and Proteins metabolism, Intracellular Signaling Peptides and Proteins genetics, Muscle Proteins genetics, Muscle Proteins metabolism

Abstract

Background: Vein grafts are commonly employed in revascularisation surgery for multivessel coronary artery disease, yet neointimal hyperplasia (NIH) remains a critical impediment to the long-term patency of these grafts. Despite this, effective methods to precisely identify and target interventions for the neointima are still inadequate., Methods: In this study, Sprague-Dawley (SD) rats were used to establish an external jugular vein transplantation model, and the NIH pathophysiological process was tracked across 11 time points (0-35 days) using various histological stains. Spatial transcriptomics was performed on normal veins and 19-day grafts to explore gene expression in neointimal regions. Immunohistochemical analysis identified neointima-specific markers, while NIH progression was assessed in SD rats with four and a half LIM domains protein 1 (Fhl1) knockout and in human saphenous veins (HSV) with adenovirus-mediated Fhl1 overexpression., Results: Typical neointimal formation commenced by day 11 postgrafting and peaked at day 19. Neointimal cells originated from newly generated α-SMA(+) repair cells located outside the grafted vein, displaying a hybrid fibroblast-smooth muscle cell phenotype. Spatial transcriptomics identified stable and sustained Fhl1 expression within the neointima throughout the entire NIH phase. Systemic knockout of Fhl1 in SD rats via the phosphoinositide 3-kinase pathway exacerbated graft inflammation, heightened cell proliferation, and accelerated NIH. Conversely, FHL1 overexpression in cultured HSV suppressed NIH., Conclusion: These findings indicate that, following grafting into the arterial system, the newly formed repair cells external to the grafted vein play a pivotal role in NIH, with neointimal cells exhibiting stable and continuous Fhl1 expression. Fhl1 serves as a protective factor against NIH both in vivo and in HSV, likely due to its anti-inflammatory and anti-proliferative effects., Key Points: This study firstly used spatial transcriptomics technique to analyse the neointima and generated a specific neointimal transcriptomic atlas. Fhl1 exhibits specific and stable expression in the spatial region of the neointima. It has thus far the highest enrichment of expression in the neointima in NIH phases, suggesting that it is a prominent molecular biomarker of neointima. We generated rats with a Fhl1 deletion and found that insufficient Fhl1 expression caused an increase in the severity of vascular inflammation and proliferation during neointimal hyperplasia. Adenovirus-mediated FHL1 overexpression in human saphenous vein have beneficial effects in preventing neointimal hyperplasia. These highlight its potential as a therapeutic target for mitigating vein graft failure associated with cardiovascular procedures. Spatial transcriptomics profiles and morphological observations demonstrated that a newly generated cell population outside the grafted vein with hybrid phenotype between SMCs and fibroblasts contributes to neointimal formation., (© 2024 The Author(s). Clinical and Translational Medicine published by John Wiley & Sons Australia, Ltd on behalf of Shanghai Institute of Clinical Bioinformatics.)

Published

2024

15. Role of four and a half LIM domain protein 1 in tumors (Review).

Author

Tao Y, Wu Y, Shen R, He S, and Miao X

Abstract

As a cytoskeletal protein, the four and a half LIM domain protein 1 (FHL1) is widely expressed in various cells, particularly skeletal and cardiac muscle cells. FHL1 is involved in the development of the skeletal muscle and myocardium, regulations of gene transcription and thyroid function, and other physiological processes. Its expression is closely related to numerous diseases, such as skeletal muscle disease and viral infections. With the advances in research, the role of FHL1 in the development of tumors is also being revealed. The mechanism of FHL1 in the regulation of tumor growth is complex and is becoming a research focus. It is also expected to become a potential target for tumor therapy. Therefore, the present article reviewed the progress in research on the role of FHL1 in cancer., Competing Interests: The authors declare that they have no competing interests., (Copyright: © 2024 Tao et al.)

Published

2024

16. Three novel FHL1 variants cause a mild phenotype of Emery‐Dreifuss muscular dystrophy.

Author

Borch, Josefine d. S., Krag, Thomas, Holm‐Yildiz, Sonja D., Cetin, Hakan, Solheim, Tuva A., Fornander, Freja, Straub, Volker, Duno, Morten, and Vissing, John

Abstract

Emery‐Dreifuss muscular dystrophy (EDMD) is a hereditary muscle disease, characterized by the clinical triade of early‐onset joint contractures, progressive muscle weakness, and cardiac involvement. Pathogenic variants in FHL1 can cause a rare X‐linked recessive form of EDMD, type 6. We report three men with novel variants in FHL1 leading to EDMD6. The onset of muscle symptoms was in late adulthood and muscle weakness was not prominent in either of the patients. All patients had hypertrophic cardiomyopathy and one of them also had cardiac arrhythmias. Western blot performed on muscle biopsies from two of the patients showed no FHL1 protein expression. We predict that the variant in the third patient also leads to the absence of FHL1 protein. Complete loss of all FHL1 isoforms combined with mild muscle involvement supports the hypothesis that loss of all FHL1 isoforms is more benign than the cytotoxic effects of expressed FHL1 protein with pathogenic missense variants. [ABSTRACT FROM AUTHOR]

Published

2022

17. Role of four and a half LIM domain protein 1 in tumors (Review).

Author

Tao, Yun, Wu, Yaxun, Shen, Rong, He, Song, and Miao, Xiaobing

Subjects

*CYTOSKELETAL proteins, *SKELETAL muscle, *MYOCARDIUM, *PROTEIN domains, *TUMOR growth

Abstract

As a cytoskeletal protein, the four and a half LIM domain protein 1 (FHL1) is widely expressed in various cells, particularly skeletal and cardiac muscle cells. FHL1 is involved in the development of the skeletal muscle and myocardium, regulations of gene transcription and thyroid function, and other physiological processes. Its expression is closely related to numerous diseases, such as skeletal muscle disease and viral infections. With the advances in research, the role of FHL1 in the development of tumors is also being revealed. The mechanism of FHL1 in the regulation of tumor growth is complex and is becoming a research focus. It is also expected to become a potential target for tumor therapy. Therefore, the present article reviewed the progress in research on the role of FHL1 in cancer. [ABSTRACT FROM AUTHOR]

Published

2025

18. An Interdisciplinary Diagnostic Approach to Guide Therapy in C3 Glomerulopathy.

Author

Schmidt, Tilman, Afonso, Sara, Perie, Luce, Heidenreich, Karin, Wulf, Sonia, Krebs, Christian F., Zipfel, Peter F., and Wiech, Thorsten

Subjects

COMPLEMENT inhibition, COMPLEMENT activation, RENAL biopsy, IMMUNOSTAINING, IMMUNOSUPPRESSION

Abstract

Since the re-classification of membranoproliferative glomerulonephritis the new disease entity C3 glomerulopathy is diagnosed if C3 deposition is clearly dominant over immunoglobulins in immunohistochemistry or immunofluorescence. Although this new definition is more orientated at the pathophysiology as mediated by activity of the alternative complement pathway C3 glomerulopathy remains a heterogenous group of disorders. Genetic or autoimmune causes are associated in several but not in all patients with this disease. However, prognosis is poorly predictable, and clinicians cannot directly identify patients that might benefit from therapy. Moreover, therapy may range from supportive care alone, unspecific immune suppression, plasma treatment, or plasma exchange to complement inhibition. The current biopsy based diagnostic approaches sometimes combined with complement profiling are not sufficient to guide clinicians neither (i) whether to treat an individual patient, nor (ii) to choose the best therapy. With this perspective, we propose an interdisciplinary diagnostic approach, including detailed analysis of the kidney biopsy for morphological alterations and immunohistochemical staining, for genetic analyses of complement genes, complement activation patterning in plasma, and furthermore for applying novel approaches for convertase typing and complement profiling directly in renal tissue. Such a combined diagnostic approach was used here for a 42-year-old female patient with a novel mutation in the Factor H gene, C3 glomerulopathy and signs of chronic endothelial damage. We present here an approach that might in future help to guide therapy of renal diseases with relevant complement activation, especially since diverse new anti-complement agents are under clinical investigation. [ABSTRACT FROM AUTHOR]

Published

2022

19. FHL1 Overexpression as A Inhibitor of Lung Cancer Cell Invasion via Increasing RhoGDIß mRNA Expression.

Author

Shi, Min-ke, Xuan, Yu-long, and He, Xiao-feng

Subjects

*LUNG cancer, *GENE expression, *PROTEIN overexpression, *CANCER cells, *CELL lines, *POLYMERASE chain reaction

Abstract

Objective: Four and a half Lin-11, Isl-1, Mac-3 (LIM) protein 1 (FHL1) is one of the FHL protein family, which is regarded as a tumor suppressor in the multiple malignant tumors. In this study, we aimed to explore the regulatory effects and mechanisms of FHL1 on lung cancer cell invasion. Materials and Methods: In this experimental study, bioinformatics analysis of FHL1 transcripts in human lung adenocarcinomas of TCGA database was performed. Quantitative real-time polymerase chain reaction (PCR) was performed to detect FHL1 mRNA expression in 15 paired human lung cancer tissues and their adjacent normal lung tissues, or lung cancer cell lines (A549 and H1299) in comparison with human bronchial epithelial cell line (Beas2B). Moreover, western blot was used to analyze FHL1 and rho GDP-dissociation inhibitor beta (RhoGDIβ) protein expression in the indicated cell lines. Also, transwell assays were employed to measure the migrated, and invaded of indicated cell lines. Results: FHL1 transcripts were downregulated in the human lung adenocarcinoma. The impaired FHL1 transcripts were positively correlated with advanced tumor node metastasis (TNM) stage. Moreover, as compared to the adjacent normal lung tissues, FHL1 mRNA was low expressed in 15 paired human lung cancer tissues than their adjacent normal lung tissues. Besides, FHL1 mRNA and protein expression were also reduced in H1299 and A549 cell lines in comparison with Beas-2B cell line. Overexpressed FHL1 protein inhibited the invasive ability of H1299 and A549 cell lines. Mechanically, FHL1 protein overexpression increased the RhoGDIβ protein and mRNA abundance, while knockdown of RhoGDIβ protein, completely restored the invasion ability of A549 (Flag-FHL1) cell line. Conclusion: Our findings indicated that as a key FHL1 downstream regulator, RhoGDIβ is in charge of FHL1 inhibiting lung cancer cell invasion abilities, providing a critical insight into understanding the role of FHL1 for lung cancer development. [ABSTRACT FROM AUTHOR]

Published

2022

20. An Interdisciplinary Diagnostic Approach to Guide Therapy in C3 Glomerulopathy

Author

Tilman Schmidt, Sara Afonso, Luce Perie, Karin Heidenreich, Sonia Wulf, Christian F. Krebs, Peter F. Zipfel, and Thorsten Wiech

Subjects

C3 glomerulopathy, membranoproliferative glomerulonephritis, complement, factor H, eculizumab, FHL1, Immunologic diseases. Allergy, RC581-607

Abstract

Since the re-classification of membranoproliferative glomerulonephritis the new disease entity C3 glomerulopathy is diagnosed if C3 deposition is clearly dominant over immunoglobulins in immunohistochemistry or immunofluorescence. Although this new definition is more orientated at the pathophysiology as mediated by activity of the alternative complement pathway C3 glomerulopathy remains a heterogenous group of disorders. Genetic or autoimmune causes are associated in several but not in all patients with this disease. However, prognosis is poorly predictable, and clinicians cannot directly identify patients that might benefit from therapy. Moreover, therapy may range from supportive care alone, unspecific immune suppression, plasma treatment, or plasma exchange to complement inhibition. The current biopsy based diagnostic approaches sometimes combined with complement profiling are not sufficient to guide clinicians neither (i) whether to treat an individual patient, nor (ii) to choose the best therapy. With this perspective, we propose an interdisciplinary diagnostic approach, including detailed analysis of the kidney biopsy for morphological alterations and immunohistochemical staining, for genetic analyses of complement genes, complement activation patterning in plasma, and furthermore for applying novel approaches for convertase typing and complement profiling directly in renal tissue. Such a combined diagnostic approach was used here for a 42-year-old female patient with a novel mutation in the Factor H gene, C3 glomerulopathy and signs of chronic endothelial damage. We present here an approach that might in future help to guide therapy of renal diseases with relevant complement activation, especially since diverse new anti-complement agents are under clinical investigation.

Published

2022

21. Novel FHL1 mutation variant identified in a patient with nonobstructive hypertrophic cardiomyopathy and myopathy – a case report

Author

Adrian Giucă, Cristina Mitu, Bogdan Ovidiu Popescu, Alexandra Eugenia Bastian, Răzvan Capşa, Adriana Mursă, Viorica Rădoi, Bogdan Alexandru Popescu, and Ruxandra Jurcuţ

Subjects

FHL1, Hypertrophic cardiomyopathy, Emery-Dreifuss muscular dystrophy, Case report, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Hypertrophic cardiomyopathy (HCM) is a genetic disorder mostly caused by sarcomeric gene mutations, but almost 10% of cases are attributed to inherited metabolic and neuromuscular disorders. First described in 2008 in an American-Italian family with scapuloperoneal myopathy, FHL1 gene encodes four-and-a-half LIM domains 1 proteins which are involved in sarcomere formation, assembly and biomechanical stress sensing both in cardiac and skeletal muscle, and its mutations are responsible for a large spectrum of neuromuscular disorders (mostly myopathies) and cardiac disease, represented by HCM, either isolated, or in conjunction with neurologic and skeletal muscle impairment. We thereby report a novel mutation variant in FHL1 structure, associated with HCM and type 6 Emery-Dreifuss muscular dystrophy (EDMD). Case presentation We describe the case of a 40 year old male patient, who was referred to our department for evaluation in the setting of NYHA II heart failure symptoms and was found to have HCM. The elevated muscular enzymes raised the suspicion of a neuromuscular disease. Rigid low spine and wasting of deltoidus, supraspinatus, infraspinatus and calf muscles were described by the neurological examination. Electromyography and muscle biopsy found evidence of chronic myopathy. Diagnosis work-up was completed by next-generation sequencing genetic testing which found a likely pathogenic mutation in the FHL1 gene (c.157-1G > A, hemizygous) involved in the development of X-linked EDMD type 6. Conclusion This case report highlights the importance of multimodality diagnostic approach in a patient with a neuromuscular disorder and associated hypertrophic cardiomyopathy by identifying a novel mutation variant in FHL1 gene. Raising awareness of non-sarcomeric gene mutations which can lead to HCM is fundamental, because of diagnostic and clinical risk stratification challenges.

Published

2020

22. Novel mutation of the FHL1 gene associated with congenital myopathy and early respiratory muscles involvement: a case report

Author

Rana Almutairi, Sara Alrashidi, Muhammed Umair, Maha Alshalan, Lamia Alsubaie, Taghrid Aloraini, Ahmed Al Ahmad, Ahmed Alfares, and Fuad Al Mutairi

Subjects

congenital myopathy, fhl1, hypotonia, congenital fiber-type disproportion myopathy, and x-linked myopathy, Genetics, QH426-470

Abstract

Background: Congenital myopathies are a diverse group of diseases that share features from the early onset of symptoms in the first year of life, such as hypotonia, muscle weakness, and developmental delays, and are often associated with respiratory insufficiency and feeding difficulties. Case presentation: Here, we report an 8-year-old boy having hypotonia and signs of respiratory insufficiency that ended with tracheostomy and ventilator-dependent status. Muscle biopsy showed histological findings of congenital fiber-type disproportion myopathy. The whole exome sequencing revealed a novel hemizygous missense variant (c.530A > C p.Gln177Pro) that confirms the diagnosis of FHL1-associated congenital myopathy. Conclusion: The findings in this study help to expand the genetic and mutational spectrum of the FHL1 gene associated with respiratory insufficiency and help in formulating a precise strategy for prognosis and future management of patients. [JBCGenetics 2020; 3(1.000): 45-51]

Published

2020

23. 结直肠癌组织ANP32A、Ataxin-3、FHL1的表达及其与肝转移的关系研究.

Author

武涛, 李强, 张旋, 丁荣, 李国钰, 夏翠峰, and 李云峰

Subjects

*COLORECTAL liver metastasis, *LYMPHATIC metastasis, *LIVER metastasis, *LIVER proteins, *LOGISTIC regression analysis, *HEPATOCELLULAR carcinoma

Abstract

Objective: To investigate the expression of acidic nuclear phosphoprotein 32A (ANP32A), Ataxin-3 and four half LIM domain proteins 1 (FHL1) in colorectal cancer and their relationship with liver metastasis. Methods: The protein levels of ANP32A, Ataxin-3 and FHL1 protein in 120 cases of colorectal cancer were detected by immunohistochemistry, the positive expression rate was analyzed. Among thems, 44 cases with liver metastasis were regarded as liver metastasis group, 76 cases without liver metastasis were re- garded as non liver metastasis group, the positive expression rates of ANP32A, Ataxin-3 and FHL1 were compared between the two groups, the influencing factors of colorectal cancer liver metastasis were analyzed, and the correlation between ANP32A, Ataxin-3 and FHL1 protein were analyzed. Results: The positive expression rate of ANP32A protein in colorectal cancer tissues was higher than that in adjacent tissues, and the positive expression rates of Ataxin-3 and FHL1 protein in colorectal cancer tissues were lower than those in adjacent tissues (P<0.05). Univariate analysis showed that the positive expression rate of ANP32A protein in liver metastasis group was significantly higher than that in non liver metastasis group, and the positive expression rates of Ataxin-3 and FHL1 protein in liver metastasis group were significantly lower than those in non liver metastasis group (P<0.05). The proportion of patients with low differentiation, T3-T4 invasion depth and lymph node metastasis in liver metastasis group was significantly higher than that in non liver metastasis group (P<0.05). Multivariate logistic regression analysis showed that positive expression of ANP32A protein, low differentiation of primary cancer, depth of invasion T3-T4 and lymph node metastasis were risk factors for liver metastasis of colorectal cancer (P<0.05). Positive expression of Ataxin-3 and FHL1 protein were protective factors for liver metastasis of colorectal cancer (P<0.05). Spearman correlation analysis showed that the positive expression rate of ANP32A was negatively correlated with the positive expression rate of Ataxin-3 and FHL1(P<0.05), and the positive expression rate of Ataxin-3 was positively correlated with the positive expression rate of FHL1 (P<0.05). Conclusion: The high expression of ANP32A and the low expression of Ataxin-3 and FHL1 are closely related to the occurrence and liver metastasis of colorectal cancer. Positive expression of ANP32A, low differentiation of primary cancer, depth of invasion T3-T4 and lymph node metastasis were risk factors for liver metastasis of colorectal cancer. Positive expression of Ataxin-3 and FHL1 protein were protective factors for liver metastasis of colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2021

24. A Dominant C150Y Mutation in FHL1 Induces Structural Alterations in LIM2 Domain Causing Protein Aggregation In Human and Drosophila Indirect Flight Muscles.

Author

Santhoshkumar, Rashmi, Preethish-Kumar, Veeramani, Mangalaparthi, Kiran K., Unni, Sruthi, Padmanabhan, Balasundaram, T. S., Keshava Prasad, Nongthomba, Upendra, Atchayaram, Nalini, and Narayanappa, Gayathri

Abstract

FHL1-related myopathies are rare X-linked dominant myopathies. Though clinically classified into several subgroups, spinal and scapuloperoneal muscle involvement are common to all. In this study, we identified c.449G > A, p.C150Y mutation by clinical exome sequencing in two patients from same family (son and mother) of Indian origin who presented with multiple contractures. Muscle biopsy showed numerous intracytoplasmic aggregates intensely stained on HE and MGT. The strong reactions to M-NBT revealed aggregates to be reducing bodies and positively labeled to anti-FHL1 antibody. Ultrastructurally, Z-band streaming and granular and granulofilamentous material were seen. Further, the translational evidence of mutant peptide was confirmed using mass spectrometric analysis. To establish p.C150Y as the cause for protein aggregation, in vivo studies were carried out using transgenic Drosophila model which highlighted Z-band abnormalities and protein aggregates in indirect flight muscles with compromised physiological function. Thus, recapitulating the X-linked human disease phenotype. Additionally, the molecular dynamics simulation analysis unraveled the drastic change in α-helix of LIM2, the region immediately next to site of C150Y mutation that could be the plausible cause for protein aggregation. To the best of our knowledge, this is the first study of p.C150Y mutation in FHL1 identified in Indian patients with in vivo and in silico analysis to establish the cause for protein aggregation in muscle. [ABSTRACT FROM AUTHOR]

Published

2021

25. Maternal smoking during pregnancy aggravated muscle phenotype in FHL1−/y offspring mice similar to congenital clubfoot through P2RX7-mediated pyroptosis.

Author

Lou, Yi, Miao, Jianing, Li, Fang, Ding, Jingjing, and Wang, Lili

Subjects

*CLUBFOOT, *CYTOSKELETAL proteins, *CIGARETTE smoke, *PREGNANCY, *MICE, *SKELETAL muscle

Abstract

[Display omitted] • Maternal smoking aggravated muscle phenotype in FHL1−/y offspring mice. • P2RX7-mediated pyroptosis participated in aggravated muscle phenotype. • Cytoskeletal proteins-MYBPC2, LDB3 involved in aggravated muscle phenotype. Congenital clubfoot (CCF) is a common birth defect. Maternal smoking during pregnancy increases the risk of CCF. In previous research, we found muscle phenotypes similar to CCF in four and a half LIM domain protein 1 (FHLI) offspring mice (FHL1−/y). However, the role of P2RX7-mediated pyroptosis in the effect of cigarette smoke (CS) on the skeletal muscle of FHL1−/y mice during pregnancy is unclear. In the present study, pregnant mice at 11 days of gestation were exposed to CS and male offspring of wild-type (WT) and FHL1−/y mice were divided into four groups (Control-WT, Control-KO, CS-WT, CS-KO). The histomorphology of lower limb muscles was examined using hematoxylin and eosin (H&E) staining. P2RX7, indicators of pyroptosis (NLRP3, ASC, cleaved-caspase 1, IL-1β), and cytoskeletal proteins (MYBPC2, LDB3) were also detected using immunoblotting. CS exposure during pregnancy aggravated the muscle phenotype similar to CCF in FHL1−/y offspring mice. FHL1 gene knockout (KO) or CS exposure during pregnancy each activated the expression of P2RX7, cell pyroptosis-related proteins (NLRP3, ASC, cleaved-caspase 1, IL-1β), a muscle injury marker (MYOD1), and cytoskeletal proteins (MYBPC2, LDB3); these two factors had an additive effect. The results showed maternal smoking during pregnancy aggravated muscle phenotype similar to CCF in FHL 1 −/y offspring mice through P2RX7-mediated pyroptosis. [ABSTRACT FROM AUTHOR]

Published

2021

26. FHL1 promotes glioblastoma aggressiveness through regulating EGFR expression.

Author

Sun, Lili, Chen, Lili, Zhu, Hua, Li, Yumo, Chen, Clark C., and Li, Ming

Subjects

*EPIDERMAL growth factor receptors, *TRANSCRIPTION factor Sp1, *GLIOBLASTOMA multiforme

Abstract

The four‐and‐a‐half LIM domain protein 1 (FHL1) plays a key role in multiple cancers. Here, we characterized its role in glioblastoma (GBM), the most common and incurable form of brain cancer. Overexpression of FHL1 promotes growth, migration, and invasion of GBM cells in vivo and in vitro. In contrast, FHL1 silencing by RNAi exhibits the opposite effects. FHL1 interacts with the transcription factor SP1 to upregulate epidermal growth factor receptor (EGFR) expression and activate the downstream signaling cascades, including Src, Akt, Erk1/2, and Stat3, leading to GBM malignancy. FHL1 is highly expressed and positively correlated with EGFR levels in human GBM, particularly those of the classical subtype. Our results suggest that the FHL1‐SP1‐EGFR axis plays a tumor‐promoting role, and highlight the translational potential of inhibiting FHL1 for GBM treatment. [ABSTRACT FROM AUTHOR]

Published

2021

27. Structural and Functional Characterization of Host FHL1 Protein Interaction with Hypervariable Domain of Chikungunya Virus nsP3 Protein.

Author

Lukash, Tetyana, Agback, Tatiana, Dominguez, Francisco, Shiliaev, Nikita, Meshram, Chetan, Frolova, Elena I., Agback, Peter, and Frolov, Ilya

Subjects

*VIRAL proteins, *PROTEIN-protein interactions, *NUCLEAR magnetic resonance, *CHIKUNGUNYA virus, *CARRIER proteins, *PROTEIN domains

Abstract

Decades of insufficient control have resulted in unprecedented spread of chikungunya virus (CHIKV) around the globe, and millions have suffered from the highly debilitating disease. Nevertheless, the current understanding of CHIKV-host interactions and adaptability of the virus to replication in mosquitoes and mammalian hosts is still elusive. Our new study shows that four-and-a-half LIM domain protein (FHL1) is one of the host factors that interact with the hypervariable domain (HVD) of CHIKV nsP3. Unlike G3BPs, FHL1 is not a prerequisite of CHIKV replication, and many commonly used cell lines do not express FHL1. However, its expression has a detectable stimulatory effect(s) on CHIKV replication, and Fhl1 knockout (KO) cell lines demonstrate slower infection spread. Nuclear magnetic resonance (NMR)-based studies revealed that the binding site of FHL1 in CHIKV nsP3 HVD overlaps that of another proviral host factor, CD2AP. The structural data also demonstrated that FHL1-HVD interaction is mostly determined by the LIM1 domain of FHL1. However, it does not mirror binding of the entire protein, suggesting that other LIM domains are involved. In agreement with previously published data, our biological experiments showed that interactions of CHIKV HVD with CD2AP and FHL1 have additive effects on the efficiency of CHIKV replication. This study shows that CHIKV mutants with extensive modifications of FHL1- or both FHL1- and CD2AP-binding sites remain viable and develop spreading infection in multiple cell types. Our study also demonstrated that other members of the FHL family can bind to CHIKV HVD and thus may be involved in viral replication. [ABSTRACT FROM AUTHOR]

Published

2021

28. Anti-FHL1 autoantibodies in adult patients with myositis: a longitudinal follow-up analysis.

Author

Galindo-Feria AS, Lodin K, Horuluoglu B, Sarrafzadeh-Zargar S, Wigren E, Gräslund S, Danielsson O, Wahren-Herlenius M, Dastmalchi M, and Lundberg IE

Abstract

Objectives: To determine prevalence and clinical associations of anti-FHL1 autoantibodies in patients with idiopathic inflammatory myopathies (IIM), and to evaluate autoantibody levels over time., Methods: Sera at the time of diagnosis from patients with IIM (n = 449), autoimmune disease controls (DC, n = 130), neuromuscular diseases (NMD, n = 16) and healthy controls (HC, n = 100) were analyzed for anti-FHL1 autoantibodies by Enzyme-Linked ImmunoSorbent Assay (ELISA). Patients with IIM FHL1+ and FHL1- were included in a longitudinal analysis. Serum levels were correlated to disease activity., Results: Autoantibodies to FHL1 were more frequent in patients with IIM (122/449, 27%) compared with DC (Autoimmune DC and NMD, 13/146, 9%, p< 0.001) and HC (3/100,3%, p< 0.001). Anti-FHL1 levels were higher in IIM [median (IQR)=0.62 (0.15-1.04)] in comparison with DC [0.22 (0.08-0.58)], HC [0.35 (0.23-0.47)] and NMD [0.48 (0.36-0.80)] p< 0.001. Anti-FHL1+ patients with IIM were younger at time of diagnosis compared with the anti-FHL1- group (p= 0.05) and were seronegative for other autoantibodies in 25%.In the first follow-up anti-FHL1+ sample 20/33 (60%) positive at baseline had turned negative for anti-FHL1 autoantibodies. Anti-FHL1 autoantibodies rarely appeared after initiating treatment. Anti-FHL1 autoantibody levels correlated with CK (r = 0.62, p= 0.01), disease activity measure MYOACT (n = 14, p= 0.004) and inversely with manual muscle test-8 (r=-0.59, p= 0.02) at baseline., Conclusions: Anti-FHL1 autoantibodies were present in 27% of patients with IIM, of these 25% were negative for other autoantibodies. Other autoimmune diseases had lower frequencies and levels. Anti-FHL1 levels often decreased with immunosuppressive treatment, correlated with disease activity measures at diagnosis and rarely appeared after start of treatment., (© The Author(s) 2024. Published by Oxford University Press on behalf of the British Society for Rheumatology.)

Published

2024

29. In vitro and in silico validation of CA3 and FHL1 downregulation in oral cancer

Author

Cláudia Maria Pereira, Ana Carolina de Carvalho, Felipe Rodrigues da Silva, Matias Eliseo Melendez, Roberta Cardim Lessa, Valéria Cristina C. Andrade, Luiz Paulo Kowalski, André L. Vettore, and André Lopes Carvalho

Subjects

OSCC, Gene expression, Methylation, CA3, FHL1, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Aberrant methylation is a frequent event in oral cancer. Methods In order to better characterize these alterations, a search for genes downregulated by aberrant methylation in oral squamous cell carcinoma (OSCC) was conducted through the mining of ORESTES dataset. Findings were further validated in OSCC cell lines and patients’ samples and confirmed using TCGA data. Differentially expressed genes were identified in ORESTES libraries and validated in vitro using RT-PCR in HNSCC cell-lines and OSCC tumor samples. Further confirmation of these results was performed using mRNA expression and methylation data from The Cancer Genome Atlas (TCGA) data. Results From the set of genes selected for validation, CA3 and FHL1 were downregulated in 60% (12/20) and 75% (15/20) of OSCC samples, respectively, and in HNSCC cell lines. The treatment of cell lines JHU-13 and FaDu with the demethylating agent 5'-aza-dC was efficient in restoring CA3 and FHL1 expression. TCGA expression and methylation data on OSCC confirms the downregulation of these genes in OSCC samples and also suggests that expression of CA3 and FHL1 is probably regulated by methylation. The downregulation of CA3 and FHL1 observed in silico was validated in HNSCC cell lines and OSCC samples, showing the feasibility of integrating different datasets to select differentially expressed genes in silico. Conclusions These results showed that the downregulation of CA3 and FHL1 data observed in the ORESTES libraries was validated in HNSCC cell lines and OSCC samples and in a large cohort of samples from the TCGA database. Moreover, it suggests that expression of CA3 and FHL1 could probably be regulated by methylation having an important role the oral carcinogenesis.

Published

2018

30. Increased RNA production in Saccharomyces cerevisiae by simultaneously overexpressing FHL1, IFH1, and SSF2 and deleting HRP1.

Author

Guo, Xuewu, Zhao, Bin, Zhou, Xinran, Ni, Xiaofeng, Lu, Dongxia, Chen, Tingli, Chen, Yefu, and Xiao, Dongguang

Subjects

*SACCHAROMYCES cerevisiae, *RNA, *CELL size, *CELL growth, *STRAIN rate, *RIBOSOMES

Abstract

Ribonucleic acid (RNA) and its degradation products are widely used in the food industry. In this study, we constructed Saccharomyces cerevisiae mutants with FHL1, IFH1, SSF1, and SSF2 overexpression and HRP1 deletion, individually to evaluate the effect on RNA production. The RNA content of recombinant strains W303-1a-FHL1, W303-1a-SSF2, and W303-1a-ΔHRP1 was increased by 14.94%, 24.4%, and 19.36%, respectively, compared with the RNA content of the parent strain. However, W303-1a-IFH1 and W303-1a-SSF1 showed no significant change in RNA production compared with the parent strain. IFH1 and FHL1 encode Ifh1p and Fhl1p, respectively, which combine to form a complex that plays a key role in the transcription of the ribosomal protein (RP) gene. Ssf2p, encoded by SSF2, plays an important role in ribosome biosynthesis and Hrp1p is a negative regulator of cell growth in S. cerevisiae. Subsequently, a high RNA production strain, W112, was constructed by simultaneously overexpressing FHL1, IFH1, and SSF2 and deleting HRP1. The RNA content of W112 was 38.8% higher than the parent strain. The growth performance, RP transcription levels, and rRNA content were also investigated in the recombinant strains. This study provides a new strategy for the construction of S. cerevisiae strains containing large amounts of RNA, and it will make a significant contribution to progress in the nucleic acid industry. Key Points: • Simultaneously overexpressing FHL1, IFH1, and SSF2 and deleting HRP1 can significantly increases RNA production. • The production of RNA increased by 38.8% in Saccharomyces cerevisiae. • The cell size and growth rate of the strains with higher RNA content also increased. [ABSTRACT FROM AUTHOR]

Published

2020

31. FHL1 regulates myoblast differentiation and autophagy through its interaction with LC3.

Author

Han, Shunshun, Cui, Can, He, Haorong, Shen, Xiaoxu, Chen, Yuqi, Wang, Yan, Li, Diyan, Zhu, Qing, and Yin, Huadong

Subjects

*MYOBLASTS, *MUSCLE growth, *SKELETAL muscle, *MYOCARDIUM, *PROTEIN domains, *ADP-ribosyltransferases

Abstract

Four and a half LIM domain protein 1 (FHL1) belongs to the FHL protein family and is predominantly expressed in skeletal and cardiac muscle. FHL1 acts as a scaffold during sarcomere assembly and plays a vital role in muscle growth and development. Autophagy is key to skeletal muscle development and regeneration, with its dysfunction associated with a range of muscular pathologies and disorders. In this study, we constructed FHL1‐silenced or FHL1‐overexpressed myoblasts to investigate its role in autophagy during the differentiation of chicken myoblasts into myotubules. Our data showed that FHL1 contributes to myoblast differentiation as measured through MyoG, MyoD, Myh3, and Mb mRNA expression, MyoG and MyHC protein expression and the morphological characteristics of myoblasts. The results showed that FHL1 silencing inhibited the expression of ATG5 and ATG7, meanwhile, immunofluorescence and immunoprecipitation showed that FHL1 and LC3 interacted to regulate the correct formation of autophagosomes. FHL1 inhibition increased cleaved caspase‐3 and PARP abundance and promoted myoblast apoptosis. Furthermore, FHL1 rescued skeletal muscle atrophy through regulating the expression of Atrogin‐1 and MuRF1. Taken together, these data suggested that FHL1 regulates chicken myoblast differentiation through its interaction with LC3. [ABSTRACT FROM AUTHOR]

Published

2020

32. FHL1‐mutated reducing body myopathy.

Author

Lim, Ka Young, Kim, Hyun Hee, Sung, Jung‐Joon, Oh, Byung‐Mo, Kim, Keewon, and Park, Sung‐Hye

Subjects

*MUSCLE diseases, *MUSCLE weakness, *MAGNETIC resonance imaging, *MISSENSE mutation, *NEURAL conduction, *MYOFIBRILS

Abstract

Here, we report about reducing body myopathy, associated with a mutation in the four and a half LIM domain 1 gene (FHL1), identified in a 40‐year‐old woman who was suffering from subtle muscle weakness since the age of six and a limping gait since the age of 22 years. In addition to her elevated muscle enzyme level and magnetic resonance imaging, myopathy was highly suspected considering progression of symptoms. Nerve conduction studies and electromyogram suggested myopathy. The muscle biopsy revealed severe dystrophic features with many reducing bodies on hematoxylin and eosin, nicotinomide adenine dinucleotide dehydrogenase‐tetrazolium reductase (NADH‐TR), and modified Gomori stains and ubiquitin immunohistochemistry. Whole‐exome sequencing revealed Xq26.3 encoding FHL1 missense mutations (NM_001159704) in exon 4: p.C150R, c.T448C. FHL1‐mutated "reducing body myopathy" is worth reporting based on its rarity and unique clinicopathologic features including ultrastructure. The confirmative diagnosis is still very difficult before gene analysis because clinical and pathological features of this disease overlap with other myofibrillar myopathies. We stress the importance of genotype‐phenotype correlation to obtain a precise diagnosis. [ABSTRACT FROM AUTHOR]

Published

2020

33. Muscle death participates in myofibrillar abnormalities in FHL1 knockout mice.

Author

Ding, Jingjing, Cong, Yanfei, Li, Fang, Liu, Bo, Wu, Di, Miao, Jianing, and Wang, Lili

Subjects

*KNOCKOUT mice, *NEMALINE myopathy, *HUMAN abnormalities, *SKELETAL muscle, *CELL death, *TIBIALIS anterior, *MUSCLES, *MYOFIBROBLASTS

Abstract

Mutations in the four and-a-half LIM domain protein 1 (FHL1) gene or FHL1 protein deletion have been identified as the cause of rare hereditary myopathies or cardiomyopathies. In our previous study, autophagy activation was associated with myofibrillar abnormalities in FHL1 knockout (KO) mice. P2RX7 induces cell death, such as autophagy, pyroptosis or apoptosis via cell-specific downstream signaling; however, the roles of P2RX7 in pyroptosis or apoptosis in myofibrillar abnormalities in FHL1 KO mice have not been well elucidated. In this study, skeletal muscle and heart of 2.5 months old WT and FHL1 KO male mice histomorphology were examined by hematoxylin and eosin staining. The indicators for pyroptosis (NLRP3; ASC; cleaved-caspase1; IL-1β), apoptosis (Apaf-1; Bcl-2; caspase9; cleaved-caspase3), and P2RX7 were detected in the triceps (Tri), tibialis anterior muscles (TA), and heart by western blot and/or immunohistochemistry in WT and FHL1 KO male mice. Indicators for pyroptosis (ASC; cleaved-caspase1; IL-1β) and apoptosis (Apaf-1 and cleaved-caspase3), as well as P2RX7 were upregulated in Tri, tibialis TA, and heart in FHL1 KO mice, indicating pyroptosis and apoptosis play important roles in myofibrillar abnormalities in FHL1 KO mice. P2RX7 may participate in myofibrillar abnormalities by activating pyroptosis and apoptosis in FHL1 KO mice. These findings have basic implications for the understanding of myopathies induced by FHL1 deficiency and provide new avenues for the treatment of these hereditary myopathies by modulating P2RX7. • The absence of FHL1 causes myofibrillar abnormalities. • Myofibrillar abnormalities may be induced by enhanced pyroptosis and apoptosis. • The enhanced pyroptosis and apoptosis may be regulated by P2RX7 in FHL1 KO mice. • HSP90 might participate in the myofibrillar abnormalities in FHL1 KO mice. [ABSTRACT FROM AUTHOR]

Published

2020

34. FHL1-related myopathy may not be classified by reducing bodies in muscle biopsy.

Author

Chen, Ting, Lu, Xianghui, Shi, Qiang, Guo, Junhong, Wang, Huifang, Wang, Qian, Yin, Xi, Zhang, Yutong, Pu, Chuanqiang, and Zhou, Dong

Subjects

*POSTURAL muscles, *FACIOSCAPULOHUMERAL muscular dystrophy, *MUSCLE weakness, *MUSCLE diseases, *MUSCULAR dystrophy, *NEMALINE myopathy, *MUSCLES

Abstract

• We identified a novel FHL1 gene mutation. • Muscle biopsy showed reducing bodies in an XMPMA patient. • We provide the first report of four FHL1-related myopathy patients from China. FHL1-related myopathies, including reducing body myopathy (RBM), X-linked scapulo-axio-peroneal myopathy, rigid spine syndrome, X-linked myopathy with postural muscle atrophy (XMPMA), X-linked Emery–Dreifuss muscular dystrophy and hypertrophic cardiomyopathy, are clinically and pathologically heterogeneous disorders caused by FHL1 gene mutations. According to previous reports, the first three types are myopathies with reducing bodies observed in biopsies, and the last three are myopathies without reducing bodies. We report four FHL1-related myopathy patients, including an XMPMA patient and a RBM family with three patients. Clinical information, muscle biopsies, electromyograms and genetic testing were obtained. Muscle weakness and atrophy, spinal rigidity, and joint contracture were present in the RBM family. The XMPMA patient showed a pseudoathletic appearance with muscle weakness and atrophy, spinal rigidity and deformity. The index patient of the RBM family underwent two muscle biopsies to find reducing bodies. Interestingly, these muscle biopsies revealed reducing bodies and rimmed vacuoles not only in the RBM family but also in the XMPMA patient. Next-generation sequencing identified a reported single missense mutation c.448 C>T (p. C150R) in the RBM family and a novel mutation c.814T>C (p. S272P) in the XMPMA patient. Therefore, FHL1-related myopathies overlap substantially and may not be simply classified into subtypes depending on reducing bodies. Biopsies of additional affected muscles can aid in finding reducing bodies. We report the first XMPMA patient with a novel FHL1 mutation and reducing bodies in a muscle biopsy in China. [ABSTRACT FROM AUTHOR]

Published

2020

35. Concurrent positive anti-3-hydroxy-3-methylglutaryl-coenzyme a reductase antibody with reducing body myopathy: Possible double trouble.

Author

Tanboon, Jantima, Sanmaneechai, Oranee, Charuvanij, Sirirat, Sangruchi, Tumtip, Galindo-Feria, Angeles S., Lundberg, Ingrid E., Ohnuki, Yuko, Shiina, Takashi, Suzuki, Shigeaki, and Nishino, Ichizo

Subjects

*NEMALINE myopathy, *ARTHROGRYPOSIS, *MUSCLE diseases, *LEFT ventricular hypertrophy, *MUSCLE weakness, *MUSCULAR dystrophy, *CREATINE kinase

Abstract

• We report anti-HMGCR antibody positivity with reducing body myopathy in a 6-year-old boy. • Unusual clinical and pathological features could be a mixed result of two entities. • Comprehensive workup lead to the "possible double-trouble" diagnosis. Anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase myopathy is less common in children but has been associated with more favorable prognosis than adult patients after immunotherapies. We report anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase antibody positivity in a 6-year-old boy with progressive muscle weakness, scoliosis, spinal rigidity, multiple joint contractures, mild left ventricular hypertrophy, and elevated serum creatine kinase. In contrast to most of previously reported pediatric anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase myopathy, he showed little response to immunotherapies. Muscle biopsy contained changes suggestive of myofiber necrosis and regeneration and reducing bodies. The diagnosis of reducing body myopathy was later confirmed by reported c.368A> G (p.His123Arg) mutation in the FHL1 gene. Although the level of association between these two conditions is still inconclusive, this is the first report of concurrent positive anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase antibody with reducing body myopathy emphasizing the possibility of co-occurrence of immune mediated necrotizing myopathy and muscular dystrophy and importance of comprehensive diagnostic investigations in unusual cases. [ABSTRACT FROM AUTHOR]

Published

2019

36. Emery–Dreifuss muscular dystrophy: a test case for precision medicine

Author

Pillers DAM and Von Bergen NH

Subjects

emerin, FHL1, Lamins A/C, nuclear envelope, Medicine (General), R5-920, Genetics, QH426-470

Abstract

De-Ann M Pillers,1 Nicholas H Von Bergen21Division of Neonatology and Newborn Medicine, 2Division of Cardiology, Department of Pediatrics, University of Wisconsin-Madison, Madison, WI, USAAbstract: Emery–Dreifuss muscular dystrophy (EDMD) is characterized by the clinical triad of scapulohumeroperoneal muscle weakness, joint contractures, and cardiac defects that include arrhythmias and dilated cardiomyopathy. Although there is a defining group of clinical findings, the proteins responsible and their underlying gene defects leading to EDMD are varied. A common aspect of the gene defects is their involvement in, or with, the nuclear envelope. Treatment approaches are largely based on clinical symptoms. The genetic diversity of EDMD predicts that a cure will ultimately depend upon the individual's defect at the gene level, making this an ideal candidate for a precision medicine approach.Keywords: emerin, FHL1, lamins A/C, nuclear envelope

Published

2016

37. Aberrant Protein Turn-Over Associated With Myofibrillar Disorganization in FHL1 Knockout Mice

Author

Jingjing Ding, Yan Fei Cong, and Bo Liu

Subjects

FHL1, protein turn-over, autophagy, myopathy, myofibrillar disorganization, Genetics, QH426-470

Abstract

Mutations in the FHL1 gene, and FHL1 protein deletion, are associated with rare hereditary myopathies and cardiomyopathies. FHL1-null mice develop age-dependent myopathy and increased autophagic activity. However, the molecular pathway involved in contractile function and increased autophagic activity in the FHL1-null mouse has not yet been fully elucidated. In this study, FHL1 protein was knocked out in mice using Transcription Activator-like Effector Nucleases (TALENs) and the IRS1-FOXO1/mTOR signaling pathway was investigated in skeletal muscles and heart. TALEN constructs caused targeted mutations in 30% of newborn mice; these mutations caused a deletion of 1–13 base pairs which blocked synthesis of the full-length FHL1 protein. Furthermore, 2.5-month old FHL1-null male mice were not prone to global muscular fatigue when compared with WT littermates, but histological analysis and ultrastructural analysis by transmission electron microscopy confirmed the presence of myofibrillar disorganization and the accumulation of autophagosome or autolysosome-like structures in FHL1-null mice. Moreover, autophagy and mitophagy were both activated in FHL1 KO mice and the degradation of autophagic lysosomes was impeded. Enhanced autophagic activity in FHL1 KO mice was induced by FOXO1 up-regulation and protein synthesis was increased via mTOR. The cytoskeletal proteins, MYBPC2 and LDB3, were involved in the formation of pathological changes in FHL1 KO mice. Markers of early differentiation (MEF2C and MYOD1) and terminal differentiation (total MYH) were both up-regulated in tibialis anterior (TA) muscles in FHL1 KO mice. The number of type I and type II fibers increased in FHL1-null TA muscles, but the number of type| | b, and type | | d fibers were both reduced in FHL1-null TA muscles. The results obtained from the heart were consistent with those from the skeletal muscle and indicated autophagic activation by FOXO1 and an increase in protein synthesis via mTOR also occurred in the heart tissue of FHL1 knockout mice. In conclusion, aberrant protein turn-over associated with myofibrillar disorganization in FHL1 knockout mice. the up-regulation of FOXO1 was associated with enhanced autophagic activity and pathological changes in the muscle fibers of FHL1 KO mice. These results indicated that autophagy activated by FOXO1 is a promising therapeutic target for hereditary myopathies and cardiomyopathies induced by FHL1.

Published

2018

38. A New Host Factor Essential for Chikungunya Virus.

Author

Schnierle, Barbara S.

Subjects

*VIRAL proteins, *VIRAL replication, *DRUG development, *CHIKUNGUNYA virus, *TARGETED drug delivery

Abstract

FHL1 has been identified as a host protein that is essential for chikungunya virus (CHIKV) replication. FHL1 interacts with the chikungunya non-structural protein 3, which is thought to recruit cellular proteins to the viral replication complex. Inhibition of this interaction is a promising target for drug development. [ABSTRACT FROM AUTHOR]

Published

2020

39. FHL1 activates myostatin signalling in skeletal muscle and promotes atrophy

Author

Jen Y. Lee, Dede Lori, Dominic J. Wells, and Paul R. Kemp

Subjects

Muscle wasting, Fibre type, FHL1, Myostatin, Mouse, Biology (General), QH301-705.5

Abstract

Myostatin is a TGFβ family ligand that reduces muscle mass. In cancer cells, TGFβ signalling is increased by the protein FHL1. Consequently, FHL1 may promote signalling by myostatin. We therefore tested the ability of FHL1 to regulate myostatin function. FHL1 increased the myostatin activity on a SMAD reporter and increased myostatin dependent myotube wasting. In mice, independent expression of myostatin reduced fibre diameter whereas FHL1 increased fibre diameter, both consistent with previously identified effects of these proteins. However, co‐expression of FHL1 and myostatin reduced fibre diameter to a greater extent than myostatin alone. Together, these data suggest that the expression of FHL1 may exacerbate muscle wasting under the appropriate conditions.

Published

2015

40. Aberrant Protein Turn-Over Associated With Myofibrillar Disorganization in FHL1 Knockout Mice.

Author

Ding, Jingjing, Cong, Yan Fei, Liu, Bo, Miao, Jianing, and Wang, Lili

Subjects

MUSCLE diseases, LABORATORY mice, MUSCLE fatigue

Abstract

Mutations in the FHL1 gene, and FHL1 protein deletion, are associated with rare hereditary myopathies and cardiomyopathies. FHL1-null mice develop age-dependent myopathy and increased autophagic activity. However, the molecular pathway involved in contractile function and increased autophagic activity in the FHL1-null mouse has not yet been fully elucidated. In this study, FHL1 protein was knocked out in mice using Transcription Activator-like Effector Nucleases (TALENs) and the IRS1-FOXO1/mTOR signaling pathway was investigated in skeletal muscles and heart. TALEN constructs caused targeted mutations in 30% of newborn mice; these mutations caused a deletion of 1–13 base pairs which blocked synthesis of the full-length FHL1 protein. Furthermore, 2.5-month old FHL1-null male mice were not prone to global muscular fatigue when compared with WT littermates, but histological analysis and ultrastructural analysis by transmission electron microscopy confirmed the presence of myofibrillar disorganization and the accumulation of autophagosome or autolysosome-like structures in FHL1-null mice. Moreover, autophagy and mitophagy were both activated in FHL1 KO mice and the degradation of autophagic lysosomes was impeded. Enhanced autophagic activity in FHL1 KO mice was induced by FOXO1 up-regulation and protein synthesis was increased via mTOR. The cytoskeletal proteins, MYBPC2 and LDB3, were involved in the formation of pathological changes in FHL1 KO mice. Markers of early differentiation (MEF2C and MYOD1) and terminal differentiation (total MYH) were both up-regulated in tibialis anterior (TA) muscles in FHL1 KO mice. The number of type I and type II fibers increased in FHL1-null TA muscles, but the number of type| | b, and type | | d fibers were both reduced in FHL1-null TA muscles. The results obtained from the heart were consistent with those from the skeletal muscle and indicated autophagic activation by FOXO1 and an increase in protein synthesis via mTOR also occurred in the heart tissue of FHL1 knockout mice. In conclusion, aberrant protein turn-over associated with myofibrillar disorganization in FHL1 knockout mice. the up-regulation of FOXO1 was associated with enhanced autophagic activity and pathological changes in the muscle fibers of FHL1 KO mice. These results indicated that autophagy activated by FOXO1 is a promising therapeutic target for hereditary myopathies and cardiomyopathies induced by FHL1. [ABSTRACT FROM AUTHOR]

Published

2018

41. A zebrafish model for FHL1-opathy reveals loss-of-function effects of human FHL1 mutations.

Author

Keßler, M., Kieltsch, A., Kayvanpour, E., Katus, H.A., Schoser, B., Schessl, J., Just, S., and Rottbauer, W.

Subjects

*MISSENSE mutation, *OLIGONUCLEOTIDES, *LOGPERCH, *EMBRYOS, *MYOCARDIUM

Abstract

Missense mutations in the four and a half LIM domain 1 ( FHL1 ) gene were found to cause X-linked inherited myopathies of both skeletal and heart muscles. However, the mechanisms by which FHL1 mutations impact on FHL1 function and lead to alteration of muscle structure and function have not been deciphered yet. We generated here by Morpholino-modified antisense oligonucleotide-mediated gene knockdown fHL1-deficient zebrafish embryos. Similar to the human situation, fhl1a -morphants zebrafish displayed severe skeletal and heart muscle myopathy. Whereas ectopic expression of wild-type FHL1 (FHL1 wt) suppressed both skeletal and heart muscle myopathy in fhl1a -morphants zebrafish, overexpression of the FHL1-opathy associated human mutations FHL1 -H123Y, FHL1 -C132F or FHL1 -C224W did not rescue skeletal and heart muscle myopathy in fhl1a -morphants. Overexpression of FHL1 -H123Y, FHL1 -C132F or FHL1 -C224W in wild-type zebrafish did not induce myopathy in a dominant-negative mode. Altogether these results indicate that FHL1 mutations found to cause X-linked FHL1-opathies in humans consistently lead to severely impaired FHL1 function. [ABSTRACT FROM AUTHOR]

Published

2018

42. FHL1对肺腺癌细胞株A549生物学特性的影响.

Author

季春华, 刘辉, and 向明

Abstract

Objective To explore the effect of expression of FHL1 on biological character of lung adenocarcinoma cell line A549. Methods Lung adenocarcinoma cell line A549 was transfected by FHL1 mRNA and shRNA lentivirus vector. The stable overexpression of FHL1 in lung adenocarcinoma cell line A549 model and low expression of cell line model were tested by Western blot and RT-PCR method.CCK-8 test, Transwell invasion, flow cytometry and Colony-forming Assay were used to test the proliferation, invasion, apoptosis and anchorage independence growth of the cell line. Results The difference between the stable overexpression of FHL1 group and its low expression group was obvious tested by Western blot and RT-PCR. CCK-8 test showed higher cell proliferation of the low expression group than that of the overexpression group and the blank group (P=0.002 2). Flow cytometry showed that the apoptosis rate of the overexpression group was 50.48%, significantly higher than that of the two low expression groups (16.41%, 20.12%) and blank group (25.90%, P<0.001). The invasiveness of the overexpression group was obviously lower than the low expression group and blank group in the Transwell invasion (P<0.001). Colony-forming Assay showed that the colony number of the overexpression group was 28.7±6.0, significantly less than the two low expression groups (157.0±6.4, 150.7±9.5, P<0.000 1). Conclusions The stable overexpression and low expression of FHL1 in lung cancer cell line A549 models were successfully constructed. The overexpression of FHL1 inhibited the proliferation, invasion and metastasis, and accelerated apoptosis in lung adenocarcinoma cell line A549. [ABSTRACT FROM AUTHOR]

Published

2018

43. Reducing body myopathy – A new pathogenic FHL1 variant and literature review

Author

Isabella Araújo Mota, Pedro Nogueira Fontana, Alzira Alves de Siqueira Carvalho, and Carolina da Cunha Correia

Subjects

Adult, Male, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Adolescent, Biopsy, Mutation, Missense, Muscle Proteins, Reducing body myopathy, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Muscular Diseases, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Child, Muscle, Skeletal, Genetics (clinical), Muscle biopsy, medicine.diagnostic_test, biology, business.industry, Intracellular Signaling Peptides and Proteins, Genetic Diseases, X-Linked, Progressive muscle weakness, LIM Domain Proteins, Middle Aged, FHL1, Pedigree, Phenotype, 030104 developmental biology, Neurology, Severe phenotype, Child, Preschool, Mutation, Pediatrics, Perinatology and Child Health, biology.protein, Female, Creatine kinase, Neurology (clinical), business, 030217 neurology & neurosurgery, Progressive muscular weakness, Rare disease

Abstract

Reducing body myopathy (RBM) is a rare disease marked by progressive muscle weakness caused by a mutation in FHL1 gene. We describe a new pathogenic variant and contrasted it with 44 other cases identified in the literature. A male child presented at age 3 suffering frequent falls and progressive muscular weakness. At age 8, he was wheelchair-bound and required ventilatory support. His mother and sister died due to the same problem. Creatine kinase was 428 IU/L (190). Muscle biopsy showed typical reducing bodies, and genetic analysis identified a novel pathogenic hemizygous variant, c.370_375del. We identified 44 previous reported cases separated in two groups: 28 cases with mean age onset 7.6 ± 5 years and 16 with 26.7 ± 4.2 years. The time for the diagnosis was shorter to younger group. The initial symptoms, rigid spine, contractures, scoliosis and axial and neck weaknesses, dysphagia, cardiac involvement, were predominant in younger group. The variant c.369C G predominated in younger group and c.448T C in older one. Pathogenic variants positions seemed related to severe phenotype. Most wheelchair patients belonged to younger group. The data from this compilation and our case provided a general characterization spectrum and prognosis between two groups of age onset with RBM.

Published

2021

44. Maternal smoking during pregnancy aggravated muscle phenotype in FHL1 offspring mice similar to congenital clubfoot through P2RX7-mediated pyroptosis

Author

Yi Lou, Jianing Miao, Lili Wang, Fang Li, and Jingjing Ding

Subjects

0301 basic medicine, medicine.medical_specialty, Pregnancy, Offspring, business.industry, Pyroptosis, H&E stain, Skeletal muscle, General Medicine, P2RX7, Toxicology, medicine.disease, FHL1, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Endocrinology, medicine.anatomical_structure, Internal medicine, medicine, Gestation, business, 030217 neurology & neurosurgery

Abstract

Congenital clubfoot (CCF) is a common birth defect. Maternal smoking during pregnancy increases the risk of CCF. In previous research, we found muscle phenotypes similar to CCF in four and a half LIM domain protein 1 (FHLI) offspring mice (FHL1-/y). However, the role of P2RX7-mediated pyroptosis in the effect of cigarette smoke (CS) on the skeletal muscle of FHL1-/y mice during pregnancy is unclear. In the present study, pregnant mice at 11 days of gestation were exposed to CS and male offspring of wild-type (WT) and FHL1-/y mice were divided into four groups (Control-WT, Control-KO, CS-WT, CS-KO). The histomorphology of lower limb muscles was examined using hematoxylin and eosin (HE these two factors had an additive effect. The results showed maternal smoking during pregnancy aggravated muscle phenotype similar to CCF in FHL1-/y offspring mice through P2RX7-mediated pyroptosis.

Published

2021

45. A Dominant C150Y Mutation in FHL1 Induces Structural Alterations in LIM2 Domain Causing Protein Aggregation In Human and Drosophila Indirect Flight Muscles

Author

Veeramani Preethish-Kumar, Upendra Nongthomba, Keshava Prasad T S, Kiran K. Mangalaparthi, Sruthi Unni, Nalini Atchayaram, Balasundaram Padmanabhan, Rashmi Santhoshkumar, and Gayathri Narayanappa

Subjects

Adult, Male, Protein Conformation, alpha-Helical, 0301 basic medicine, Mutant, Mutation, Missense, Muscle Proteins, Protein aggregation, medicine.disease_cause, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Muscular Diseases, Protein Domains, medicine, Animals, Humans, Child, Muscle, Skeletal, Exome sequencing, Genes, Dominant, Mutation, Muscle biopsy, biology, medicine.diagnostic_test, Intracellular Signaling Peptides and Proteins, Genetic Diseases, X-Linked, General Medicine, LIM Domain Proteins, biology.organism_classification, Phenotype, FHL1, Cell biology, Drosophila melanogaster, 030104 developmental biology, Female, Protein Multimerization, 030217 neurology & neurosurgery

Abstract

FHL1-related myopathies are rare X-linked dominant myopathies. Though clinically classified into several subgroups, spinal and scapuloperoneal muscle involvement are common to all. In this study, we identified c.449G > A, p.C150Y mutation by clinical exome sequencing in two patients from same family (son and mother) of Indian origin who presented with multiple contractures. Muscle biopsy showed numerous intracytoplasmic aggregates intensely stained on HE and MGT. The strong reactions to M-NBT revealed aggregates to be reducing bodies and positively labeled to anti-FHL1 antibody. Ultrastructurally, Z-band streaming and granular and granulofilamentous material were seen. Further, the translational evidence of mutant peptide was confirmed using mass spectrometric analysis. To establish p.C150Y as the cause for protein aggregation, in vivo studies were carried out using transgenic Drosophila model which highlighted Z-band abnormalities and protein aggregates in indirect flight muscles with compromised physiological function. Thus, recapitulating the X-linked human disease phenotype. Additionally, the molecular dynamics simulation analysis unraveled the drastic change in α-helix of LIM2, the region immediately next to site of C150Y mutation that could be the plausible cause for protein aggregation. To the best of our knowledge, this is the first study of p.C150Y mutation in FHL1 identified in Indian patients with in vivo and in silico analysis to establish the cause for protein aggregation in muscle.

Published

2021

46. Systemic effect of FHL1 on neuromuscular junction and myotube formation via insulin-like growth factor and myostatin signaling pathways

Author

Kai Zhao, Wei Jiang, Feixu Zhang, Xia Wu, Jiamei Wu, Zengmin Du, Ying Chen, Jing Zheng, Chengyong Shen, and Xiao Xiao

Subjects

0301 basic medicine, Scaffold protein, Follistatin, Muscle Fibers, Skeletal, Neuromuscular Junction, Biophysics, Muscle Proteins, Myostatin, Biochemistry, Neuromuscular junction, Cell Line, Cell Fusion, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Receptors, Cholinergic, Phosphorylation, Molecular Biology, Cell Proliferation, Acetylcholine receptor, biology, Myogenesis, Intracellular Signaling Peptides and Proteins, Receptor Protein-Tyrosine Kinases, Cell Differentiation, Cell Biology, LIM Domain Proteins, FHL1, Cell biology, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, biology.protein, Signal transduction, Signal Transduction

Abstract

Four-and-a-half LIM domain protein 1 (FHL1) is a member of the FHL protein family that serves as a scaffold protein to maintain normal cellular structure and function. Its mutations have been implicated in multiple muscular diseases. These FHL1 related myopathies are characterized by symptoms such as progressive muscle loss, rigid or bent spine, even cardiac or respiratory failure in some patients, which implies pathological problems not only in muscles, but also in the nervous system. Moreover, decreased FHL1 protein level has been found in patients with FHL1 mutations, indicating the protein loss-of-function as a pathological cause of such diseases. These findings suggest the significance of understanding the systemic role of FHL1 in the homeostasis of nervous system and muscle. Here we reported that Fhl1 loss in C2C12 myotubes obscured acetylcholine receptor (AChR) clustering in addition to myotube fusion, which was associated with impaired MuSK phosphorylation. Mechanistically, myostatin-SMAD2/3 signaling was enhanced, whereas IGF-PI3K-AKT signaling was suppressed in Fhl1-/- C2C12 myotubes. Reversion of these molecular alterations rescued AChR clustering and differentiation deficits. These data outline a systemic regulation of AChR clustering and myotube fusion by FHL1, which may offer clues for mechanism study and development of therapeutic strategies to treat FHL1 related myopathies.

Published

2021

47. Three novel FHL1 variants cause a mild phenotype of Emery-Dreifuss muscular dystrophy

Author

Josefine d. S. Borch, Thomas Krag, Sonja D. Holm‐Yildiz, Hakan Cetin, Tuva A. Solheim, Freja Fornander, Volker Straub, Morten Duno, and John Vissing

Subjects

muscular dystrophy, Male, FHL1, Intracellular Signaling Peptides and Proteins, Muscle Proteins, LIM Domain Proteins, EDMD6, Muscular Dystrophy, Emery-Dreifuss, Phenotype, Emery-Dreifuss muscular dystrophy, Genetics, Humans, Protein Isoforms, cardiomyopathy, Genetics (clinical)

Abstract

Emery-Dreifuss muscular dystrophy (EDMD) is a hereditary muscle disease, characterized by the clinical triade of early-onset joint contractures, progressive muscle weakness, and cardiac involvement. Pathogenic variants in FHL1 can cause a rare X-linked recessive form of EDMD, type 6. We report three men with novel variants in FHL1 leading to EDMD6. The onset of muscle symptoms was in late adulthood and muscle weakness was not prominent in either of the patients. All patients had hypertrophic cardiomyopathy and one of them also had cardiac arrhythmias. Western blot performed on muscle biopsies from two of the patients showed no FHL1 protein expression. We predict that the variant in the third patient also leads to the absence of FHL1 protein. Complete loss of all FHL1 isoforms combined with mild muscle involvement supports the hypothesis that loss of all FHL1 isoforms is more benign than the cytotoxic effects of expressed FHL1 protein with pathogenic missense variants.

Published

2022

48. Effects of FHL1 and P21 on hypoxia-induced pulmonary vascular remodeling in neonatal rats.

Author

YANNA DU, JIANHUA FU, LI YAO, DAN ZHANG, NA LIU, and XINDONG XUE

Subjects

*HYPOXEMIA, *PULMONARY artery, *SPRAGUE Dawley rats, *PULMONARY hypertension, *SYSTOLIC blood pressure

Abstract

Numerous studies have demonstrated that altered expression levels of four and a half LIM domains 1 (FHL1) and P21 are necessary for hypoxia.induced pulmonary vascular remodeling in both adult rats and human patients with idiopathic pulmonary arterial hypertension. However, whether FHL1 and P21 are present in the pulmonary artery and whether these proteins affect pulmonary vascular remodeling in hypoxia.induced pulmonary hypertension (HPH) in neonatal rats remain unknown. The present study investigated the effects of altered FHL1 and P21 expression on pulmonary vascular remodeling in neonatal rats with HPH. A total of 32 newborn Sprague. Dawley rats were exposed to hypoxia or room air for 7 or 14 days (n=8/subgroup). Parameters including the percentage of medial wall thickness (WT%), the percentage of medial wall area (WA%), right ventricular (RV) mean pressure, RV hypertrophy index (RVHI) and RV systolic pressure (RVSP) were measured to evaluate the development of HPH. Additionally, the expressions of FHL1 and P21 in the pulmonary artery smooth muscle cells (PASMCs) were measured by reverse transcription.quantitative polymerase chain reaction, western blot analysis and immunohistochemical staining. WA%, WT%, RV mean pressure, RVHI and RVSP were significantly increased in the HPH model group when compared with the control group (P<0.01). The protein expression levels of FHL1 were significantly increased in the HPH group (P<0.05), while the mRNA and protein expression levels of P21 were significantly reduced (P<0.05). Pearson correlation analysis indicated that the protein expressions of FHL1 and P21 were correlated with WA% and WT% (all P<0.001), and that the protein expression of P21 was negatively correlated with that of FHL1 (P<0.01). The results indicated that the expressions of FHL1 and P21 were altered in the PASMCs of newborn rats with HPH. Furthermore, FHL1 and P21 may serve important roles in pulmonary vascular remodeling. [ABSTRACT FROM AUTHOR]

Published

2017

49. Upregulation of the Four and a Half LIM Domains 1 linked with familial venous dysplasia in a familial genetic examination.

Author

Liu J, Xie M, Duan X, Liu F, Luo P, and Liu Q

Abstract

Background: This study aimed to analyze the mutation site in a family diagnosed with venous dysplasia to identify possible pathogenic genes., Methods: A 15-year-old female presented with lower extremity venous tortuosity aggravated by ulceration. Only the young sister exhibited similar symptoms within the immediate family of the proband. Whole genome sequencing (WGS) was used to evaluate the mutation sites and chromosome copy number variations (CNV) within the family. The possible pathogenic genes located in the region with CNVs were identified, and the expression of the possible pathogenic genes was verified via quantitative polymerase chain reaction (Q-PCR) and western blotting (WB) analysis. In-vitro models were used to verify the role of possible pathogenic genes linked with the development of venous dysplasia., Results: The high-resolution karyotype analysis of the chromosomes found no abnormalities. The results of the WGS indicated that the proband and her sister shared the CNV events, including a microdeletion on chromosomes X: 13580000-1358555000 and microduplications of chromosome X: 136055000-136290000, chromosome X: 136475000-13671000. The results of the Q-PCR and WB showed that FHL1 was highly expressed in the proband and her sister, indicating that mutations of the FHL1 may have an important role in the development of vein malformations. The results of the in vitro experiments showed that FHL1 overexpression could inhibit venous development., Conclusion: The CNV in the Xq26 region (136054501-136288300) was found to be linked with the development of venous malformations in this family. However, further studies are required to evaluate the genetic mechanisms involved in the development of venous malformations., Competing Interests: None., (AJTR Copyright © 2023.)

Published

2023

50. MiR-183-5p induced by saturated fatty acids regulates the myogenic differentiation by directly targeting FHL1 in C2C12 myoblasts

Author

Wan Lee, Kyung-Ho Min, and Mai Thi Nguyen

Subjects

FHL1, Muscle Fibers, Skeletal, Gene Expression, Muscle Proteins, Muscle Development, MyoD, Biochemistry, Article, Cell Line, Myoblasts, Mice, 03 medical and health sciences, Palmitic acid, Animals, Myocyte, MEF2C, RNA, Messenger, Molecular Biology, Transcription factor, Myogenin, Cell Proliferation, 0303 health sciences, Gene knockdown, MEF2 Transcription Factors, Chemistry, Myogenesis, Fatty Acids, 030302 biochemistry & molecular biology, Intracellular Signaling Peptides and Proteins, Cell Differentiation, MicroRNA, miR-183-5p, General Medicine, LIM Domain Proteins, musculoskeletal system, Cell biology, MicroRNAs, Gene Expression Regulation, Differentiation, tissues, C2C12

Abstract

Skeletal myogenesis is a complex process that is finely regulated by myogenic transcription factors. Recent studies have shown that saturated fatty acids (SFA) can suppress the activation of myogenic transcription factors and impair the myogenic differentiation of progenitor cells. Despite the increasing evidence of the roles of miRNAs in myogenesis, the targets and myogenic regulatory mechanisms of miRNAs are largely unknown, particularly when myogenesis is dysregulated by SFA deposition. This study examined the implications of SFA-induced miR-183-5p on the myogenic differentiation in C2C12 myoblasts. Long-chain SFA palmitic acid (PA) drastically reduced myogenic transcription factors, such as myoblast determination protein (MyoD), myogenin (MyoG), and myocyte enhancer factor 2C (MEF2C), and inhibited FHL1 expression and myogenic differentiation of C2C12 myoblasts, accompanied by the induction of miR-183-5p. The knockdown of FHL1 by siRNA inhibited myogenic differentiation of myoblasts. Interestingly, miR-183-5p inversely regulated the expression of FHL1, a crucial regulator of skeletal myogenesis, by targeting the 3'UTR of FHL1 mRNA. Furthermore, the transfection of miR-183-5p mimic suppressed the expression of MyoD, MyoG, MEF2C, and MyHC, and impaired the differentiation and myotube formation of myoblasts. Overall, this study highlights the role of miR-183-5p in myogenic differentiation through FHL1 repression and suggests a novel miRNA-mediated mechanism for myogenesis in a background of obesity. [BMB Reports 2020; 53(11): 605-610].

Published

2020