Your search keyword '"mib1"' showing total 192 results

1. Structural requirements for activity of Mind bomb1 in Notch signaling

Author

Cao, Ruili, Gozlan, Oren, Airich, Alina, Tveriakhina, Lena, Zhou, Haixia, Jiang, Hanjie, Cole, Philip A., Aster, Jon C., Klein, Thomas, Sprinzak, David, and Blacklow, Stephen C.

Published

2024

2. Intricate MIB1-NOTCH-GATA6 Interactions in Cardiac Valvular and Septal Development

Author

Rebeca Piñeiro-Sabarís, Donal MacGrogan, and José Luis de la Pompa

Subjects

CHD, BAV, VSD, genetic interactions, GATA6, MIB1, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Genome-wide association studies and experimental mouse models implicate the MIB1 and GATA6 genes in congenital heart disease (CHD). Their close physical proximity and conserved synteny suggest that these two genes might be involved in analogous cardiac developmental processes. Heterozygous Gata6 loss-of-function mutations alone or humanized Mib1 mutations in a NOTCH1-sensitized genetic background cause bicuspid aortic valve (BAV) and a membranous ventricular septal defect (VSD), consistent with MIB1 and NOTCH1 functioning in the same pathway. To determine if MIB1-NOTCH and GATA6 interact in valvular and septal development, we generated compound heterozygote mice carrying different Mib1 missense (Mib1K735R and Mib1V943F) or nonsense (Mib1R530X) mutations with the Gata6STOP/+ heterozygous null mutation. Combining Mib1R530X/+ or Mib1K735R/+ with Gata6STOP/+ does not affect Gata6STOP/+ single mutant phenotypes. In contrast, combining Mib1V943F/+ with Gata6STOP/+ decreases the incidence of BAV and VSD by 50%, suggesting a suppressive effect of Mib1V943F/+ on Gata6STOP/+. Transcriptomic and functional analyses revealed that while the EMT pathway term is depleted in the Gata6STOP/+ mutant, introducing the Mib1V943F variant robustly enriches this term, consistent with the Mib1V943F/+ phenotypic suppression of Gata6STOP/+. Interestingly, combined Notch1 and Gata6 insufficiency led to a nearly fully penetrant VSD but did not affect the BAV phenotype, underscoring the complex functional relationship between MIB1, NOTCH, and GATA6 in valvular and septal development.

Published

2024

3. Sanggenon C inhibits cell proliferation and induces apoptosis by regulating the MIB1/DAPK1 axis in glioblastoma.

Author

Chang, Hongbo, Hou, Jianbing, Shao, Yaqian, Xu, Minghao, Weng, Xuelian, Du, Yi, Shi, Junbo, Zhang, Li, and Cui, Hongjuan

Subjects

FLAVONOIDS, GLIOBLASTOMA multiforme, CELL death, CELL proliferation, PROTEOMICS

Abstract

Sanggenon C (SC), a herbal flavonoid extracted from Cortex Mori, has been mentioned to possess more than one treasured organic properties. However, the molecular mechanism of its anti‐tumor impact in glioblastoma (GBM) remains unclear. In this study, we reported that SC displayed a GBM‐suppressing impact in vitro and in vivo with no apparent organ toxicity. SC dramatically suppressed cell proliferation‐induced cell apoptosis in GBM cells. Mechanistically, we unveiled that SC modulated the protein expression of death associated protain kinase 1 (DAPK1) by controlling the ubiquitination and degradation of DAPK1. Quantitative proteomic and Western blot analyses showed that SC improved DAPK1 protein degradation via decreasing the expression of E3 ubiquitin ligase Mindbomb 1 (MIB1). More importantly, the effects of SC on cell proliferation and apoptosis of GBM cells have been in part reversed through DAPK1 downregulation or MIB1 overexpression, respectively. These results indicated that SC might suppress cell proliferation and induce cell apoptosis by decreasing MIB1‐mediated DAPK1 degradation. Furthermore, we found that SC acted synergistically with temozolomide (TMZ), an anti‐cancer drug used in GBM, resulting in elevated chemotherapeutic sensitivity of GBM to TMZ. Collectively, our data suggest that SC might be a promising anti‐cancer agent for GBM therapy. [ABSTRACT FROM AUTHOR]

Published

2023

4. The E3 ubiquitin ligase MIB1 suppresses breast cancer cell migration through regulating CTNND1 protein level.

Author

Kanoh, Tohgo, Lu, Jingyu, Mizoguchi, Takamasa, and Itoh, Motoyuki

Subjects

*CANCER cell migration, *METASTATIC breast cancer, *BREAST cancer, *CELL migration, *BREAST cancer prognosis, *UBIQUITIN ligases

Abstract

Breast cancer is one of the most common invasive cancers among women. The leading cause of difficulty in treating breast cancer patients is metastasis. Because cell migration is closely related to breast cancer metastasis, elucidating the detailed mechanism by which breast cancer cells promote their migration is crucial for improving the prognosis of patients. In this study, we investigated the relationship between breast cancer cell migration and Mind bomb1 (MIB1), an E3 ubiquitin ligase. We found that the downregulation of MIB1 promotes the cell migration of MCF7, a breast cancer-derived cell line. Furthermore, knockdown of MIB1 caused a reduction in CTNND1 and thereby impaired E-cadherin membrane localization in the cell boundary region. Taken together, our data suggest that MIB1 might play a role in suppressing breast cancer cell migration. • MIB1 expression is correlated with the worse prognosis of breast cancer patients. • MIB1 suppresses cell migration in breast cancer cell lines. • MIB1 regulates CTNND1 protein level and E-cadherin localization in the cell boundary. [ABSTRACT FROM AUTHOR]

Published

2023

5. MicroRNA-198 suppresses prostate tumorigenesis by targeting MIB1

Author

Ray, Jessica, Hoey, Christianne, Huang, Xiaoyong, Jeon, Jouhyun, Taeb, Samira, Downes, Michelle R, Boutros, Paul C, and Liu, Stanley K

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Aging, Cancer, Genetics, Biotechnology, Urologic Diseases, Prostate Cancer, Aetiology, 2.1 Biological and endogenous factors, Animals, Apoptosis, Biomarkers, Tumor, Cell Proliferation, Gene Expression Regulation, Neoplastic, Humans, Male, Mice, Mice, Nude, MicroRNAs, Prognosis, Prostatic Neoplasms, Transcriptome, Tumor Cells, Cultured, Ubiquitin-Protein Ligases, Xenograft Model Antitumor Assays, microRNA, miR-198, prostate cancer, MIB1, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

MicroRNAs are small non‑coding RNA molecules which act as modulators of gene function, and have been identified as playing important roles in cancer as both tumor suppressors and oncogenes. The present study aimed to examine the role of miR‑198 in prostate cancer aggression by analyzing how it influences several hallmarks of cancer. Abundance of miR‑198 in prostate cancer and association with clinical characteristics was analyzed using a CPC‑Gene prostate cancer dataset. Overexpression of miR‑198 was performed using transient transfection of miR‑198 mimic prior to assaying proliferation, cell cycle, and colony formation in LNCaP and DU145 cell lines using standard protocols. In vivo tumor formation in athymic nude mice was examined using LNCaP xenografts with stable overexpression conferred using lentiviral miR‑198 transduction. Protein and mRNA abundance of MIB1 was determined using western blotting and RT‑qPCR respectively, while miR‑198 binding to MIB1 was validated using a luciferase reporter assay. miR‑198 abundance was lower in high Gleason grade prostate cancer relative to intermediate and low‑grade cancer. Overexpression of miR‑198 diminished proliferation of prostate cancer cell lines, increased G0/G1 cell cycle arrest, and significantly impaired colony formation. Elevated miR‑198 abundance was also demonstrated to impair tumor formation in vivo using LNCaP xenografts. Mindbomb E3 ubiquitin protein ligase 1 (MIB1) was demonstrated to be directly targeted by miR‑198, and knockdown of MIB1 recapitulated the effects of miR‑198 on proliferation and colony formation. The present evidence supports miR‑198 as an important tumor suppressor in prostate cancer, and demonstrates for the first time that it acts by targeting MIB1. The present study reinforces the importance and complexity of miRNA in regulating prostate cancer aggression.

Published

2019

6. Evaluation of the Expression Levels of Notch Signaling Pathway-Related Genes; JAG1, CXCR4, and MIB1 in Acute Myeloid Leukemia Patients

Author

Seyedeh Hananeh Ghafelehbashi, Dina Sadeghizadeh, Fatemeh Rohollah, Saghar Pahlavanneshan, and Majid Sadeghizadeh

Subjects

notch, jag1, cxcr4, mib1, acute myeloid leukemia, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background: Acute myeloid leukemia (AML) is a complex disease characterized by clonal expansion of undifferentiated myeloid precursors, resulting in impaired hematopoiesis and bone marrow failure. Different genetic and environmental factors are believed to be involved in the pathogenesis of AML. Notch signaling with a tumor suppressing plays a role in myeloproliferative disorder and is a negative regulator of myeloid progenitor commitment. Crosstalk between Notch signaling and CXCR4 axis is a matter of debate in AML.Method: In the current case-control study, we evaluated the expression level of CXCR4, JAG1, and MIB1, which are all involved or related to Notch signaling in adult AML patients. Blood samples were obtained from 25 AML and 17 healthy individuals and the expression level of the selected genes was evaluated via the real-time polymerase chain reaction.Results: Our results revealed the increased expression of JAG1, but decreased expression of CXCR4 in AML patients in Iranian population of AML patients. Moreover, some gender-associated effects on the expression of JAG1 and CXCR4 were detected, which may be related to sex hormones. The expression level of MIB1 did not change significantly. The correlation analysis showed no correlations between the age of the patients and the expression levels of the genes.Conclusion: Herein, for the first time, we suggested some new evidence regarding the complex role of Notch signaling-related genes (CXCR4 and JAG1) in the pathogenesis of AML in Iranian patients.

Published

2022

7. Acid ceramidase targeting pyruvate kinase affected trypsinogen activation in acute pancreatitis

Author

Juan Xiao, Wenying Zeng, Pengcheng Zhang, Yuan Zhou, and Qiangqiang Fang

Subjects

Acid ceramidase, MIB1, Trypsinogen, Pyruvate kinase, Acute pancreatitis, Therapeutics. Pharmacology, RM1-950, Biochemistry, QD415-436

Abstract

Abstract Background Acute pancreatitis is the sudden inflammation of the pancreas. Severe cases of acute pancreatitis are potentially fatal and have no specific treatment available. Premature trypsinogen activation could initiate acute pancreatitis. However, the mechanism underlying premature trypsinogen activation is not fully understood. Methods In this research, a primary pancreatic acinar cell or mouse acute pancreatitis model was constructed. The effect of acid ceramidase (ASAH1), which is responsible for sphingosine production, was investigated in trypsinogen activation in vitro and in vivo. Meanwhile, the proteins regulating ASAH1 or binding to sphingosine were also detected by co-immunoprecipitation followed by mass spectrometry. Results The results showed that ASAH1 increased in acute pancreatitis. Increased ASAH1 promoted the activation of trypsinogen and cathepsin B. On the contrary, ASAH1 downregulation inhibited trypsinogen and cathepsin B. Meanwhile, ASAH1 regulated the activity of trypsin and cathepsin B through sphingosine. Additionally, E3 ligase Mind bomb homolog 1 (MIB1) decreased in acute pancreatitis resulting in the decreased binding between MIB1 and ASAH1. Exogenous MIB1 diminished the elevation in trypsin activity induced by acute pancreatitis inducer. ASAH1 increased owing to the inhibition of the proteasome degradation by MIB1. In acute pancreatitis, sphingosine was found to bind to pyruvate kinase. Pyruvate kinase activation could reduce trypsinogen activation and mitochondrial reactive oxygen species (ROS) production induced by sphingosine. Conclusions In conclusion, during the process of acute pancreatitis, MIB1 downregulation led to ASAH1 upregulation, resulting in pyruvate kinase inhibition, followed by trypsinogen activation.

Published

2022

8. Sanggenon C inhibits cell proliferation and induces apoptosis by regulating the MIB1/DAPK1 axis in glioblastoma

Author

Hongbo Chang, Jianbing Hou, Yaqian Shao, Minghao Xu, Xuelian Weng, Yi Du, Junbo Shi, Li Zhang, and Hongjuan Cui

Subjects

chemosensitivity, DAPK1, glioblastoma, MIB1, sanggenon C, Medicine

Abstract

Abstract Sanggenon C (SC), a herbal flavonoid extracted from Cortex Mori, has been mentioned to possess more than one treasured organic properties. However, the molecular mechanism of its anti‐tumor impact in glioblastoma (GBM) remains unclear. In this study, we reported that SC displayed a GBM‐suppressing impact in vitro and in vivo with no apparent organ toxicity. SC dramatically suppressed cell proliferation‐induced cell apoptosis in GBM cells. Mechanistically, we unveiled that SC modulated the protein expression of death associated protain kinase 1 (DAPK1) by controlling the ubiquitination and degradation of DAPK1. Quantitative proteomic and Western blot analyses showed that SC improved DAPK1 protein degradation via decreasing the expression of E3 ubiquitin ligase Mindbomb 1 (MIB1). More importantly, the effects of SC on cell proliferation and apoptosis of GBM cells have been in part reversed through DAPK1 downregulation or MIB1 overexpression, respectively. These results indicated that SC might suppress cell proliferation and induce cell apoptosis by decreasing MIB1‐mediated DAPK1 degradation. Furthermore, we found that SC acted synergistically with temozolomide (TMZ), an anti‐cancer drug used in GBM, resulting in elevated chemotherapeutic sensitivity of GBM to TMZ. Collectively, our data suggest that SC might be a promising anti‐cancer agent for GBM therapy.

Published

2023

9. NOTCH1 Gene as a Novel Cause of Thoracic Aortic Aneurysm in Patients with Tricuspid Aortic Valve: Two Cases Reported.

Author

Torres-Juan, Laura, Rico, Yolanda, Fortuny, Elena, Pons, Jaume, Ramos, Rafael, Santos-Simarro, Fernando, Asensio, Víctor, Martinez, Iciar, and Heine-Suñer, Damian

Subjects

*THORACIC aneurysms, *AORTIC valve, *TRICUSPID valve, *MITRAL valve, *BLOOD flow

Abstract

Thoracic aortic aneurysms (TAA) consist of abnormal dilation or the widening of a portion of the ascending aorta, due to weakness or destructuring of the walls of the vessel and are potentially lethal. The congenital bicuspid aortic valve (BAV) is considered a risk factor for the development of TAA because asymmetric blood flow through the bicuspid aortic valve detrimentally influences the wall of the ascending aorta. NOTCH1 mutations have been associated with non-syndromic TAAs as a consequence of BAV, but little is known regarding its haploinsufficiency and its relationship with connective tissue abnormalities. We report two cases in which there is clear evidence that alterations in the NOTCH1 gene are the cause of TAA in the absence of BAV. On the one hand, we describe a 117 Kb deletion that includes a large part of the NOTCH1 gene and no other coding genes, suggesting that haploinsufficiency can be considered a pathogenic mechanism for this gene associated with TAA. In addition, we describe two brothers who carry two variants, one in the NOTCH1 gene and another in the MIB1 gene, corroborating the involvement of different genes of the Notch pathway in aortic pathology. [ABSTRACT FROM AUTHOR]

Published

2023

10. A novel peptide encoded by N6-methyladenosine modified circMAP3K4 prevents apoptosis in hepatocellular carcinoma

Author

Jin-Ling Duan, Wei Chen, Juan-Juan Xie, Mao-Lei Zhang, Run-Cong Nie, Hu Liang, Jie Mei, Kai Han, Zhi-Cheng Xiang, Feng-Wei Wang, Kai Teng, Ri-Xin Chen, Min-Hua Deng, Yi-Xin Yin, Nu Zhang, Dan Xie, and Mu-Yan Cai

Subjects

Hepatocellular carcinoma, circMAP3K4, N6-methyadenosine, Translation, AIF, MIB1, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Circular RNAs (circRNAs) regulate various biological activities and have been shown to play crucial roles in hepatocellular carcinoma (HCC) progression. However, only a few coding circRNAs have been identified in cancers, and their roles in HCC remain elusive. This study aimed to identify coding circRNAs and explore their function in HCC. Methods CircMAP3K4 was selected from the CIRCpedia database. We performed a series of experiments to determine the characteristics and coding capacity of circMAP3K4. We then used in vivo and in vitro assays to investigate the biological function and mechanism of circMAP3K4 and its protein product, circMAP3K4-455aa, in HCC. Results We found circMAP3K4 to be an upregulated circRNA with coding potential in HCC. IGF2BP1 recognized the circMAP3K4 N6-methyladenosine modification and promoted its translation into circMAP3K4-455aa. Functionally, circMAP3K4-455aa prevented cisplatin-induced apoptosis in HCC cells by interacting with AIF, thus protecting AIF from cleavage and decreasing its nuclear distribution. Moreover, circMAP3K4-455aa was degraded through the ubiquitin–proteasome E3 ligase MIB1 pathway. Clinically, a high level of circMAP3K4 is an independent prognostic factor for adverse overall survival and adverse disease-free survival of HCC patients. Conclusions CircMAP3K4 is a highly expressed circRNA in HCC. Driven by m6A modification, circMAP3K4 encoded circMAP3K4-455aa, protected HCC cells from cisplatin exposure, and predicted worse prognosis of HCC patients. Targeting circMAP3K4-455aa may provide a new therapeutic strategy for HCC patients, especially for those with chemoresistance. Graphical Abstract CircMAP3K4 is a highly expressed circRNA in HCC. Driven by m6A modification, IGF2BP1 facilitates circMAP3K4 peptide translation, then the circMAP3K4 peptide inhibits AIF cleavage and nuclear distribution, preventing HCC cells from cell death under stress and promoting HCC progression.

Published

2022

11. Human Hereditary Cardiomyopathy Shares a Genetic Substrate With Bicuspid Aortic Valve.

Author

Siguero-Álvarez, Marcos, Salguero-Jiménez, Alejandro, Grego-Bessa, Joaquim, de la Barrera, Jorge, MacGrogan, Donal, Prados, Belén, Sánchez-Sáez, Fernando, Piñeiro-Sabarís, Rebeca, Felipe-Medina, Natalia, Torroja, Carlos, Gómez, Manuel José, Sabater-Molina, María, Escribá, Rubén, Richaud-Patin, Ivonne, Iglesias-García, Olalla, Sbroggio, Mauro, Callejas, Sergio, O'Regan, Declan P., McGurk, Kathryn A., and Dopazo, Ana

Subjects

*MITRAL valve, *AORTIC valve, *RECESSIVE genes, *CARDIAC magnetic resonance imaging, *GAIN-of-function mutations, *GENE expression, *GENE expression profiling, *AORTIC valve insufficiency

Abstract

Background: The complex genetics underlying human cardiac disease is evidenced by its heterogenous manifestation, multigenic basis, and sporadic occurrence. These features have hampered disease modeling and mechanistic understanding. Here, we show that 2 structural cardiac diseases, left ventricular noncompaction (LVNC) and bicuspid aortic valve, can be caused by a set of inherited heterozygous gene mutations affecting the NOTCH ligand regulator MIB1 (MINDBOMB1) and cosegregating genes.Methods: We used CRISPR-Cas9 gene editing to generate mice harboring a nonsense or a missense MIB1 mutation that are both found in LVNC families. We also generated mice separately carrying these MIB1 mutations plus 5 additional cosegregating variants in the ASXL3, APCDD1, TMX3, CEP192, and BCL7A genes identified in these LVNC families by whole exome sequencing. Histological, developmental, and functional analyses of these mouse models were carried out by echocardiography and cardiac magnetic resonance imaging, together with gene expression profiling by RNA sequencing of both selected engineered mouse models and human induced pluripotent stem cell-derived cardiomyocytes. Potential biochemical interactions were assayed in vitro by coimmunoprecipitation and Western blot.Results: Mice homozygous for the MIB1 nonsense mutation did not survive, and the mutation caused LVNC only in heteroallelic combination with a conditional allele inactivated in the myocardium. The heterozygous MIB1 missense allele leads to bicuspid aortic valve in a NOTCH-sensitized genetic background. These data suggest that development of LVNC is influenced by genetic modifiers present in affected families, whereas valve defects are highly sensitive to NOTCH haploinsufficiency. Whole exome sequencing of LVNC families revealed single-nucleotide gene variants of ASXL3, APCDD1, TMX3, CEP192, and BCL7A cosegregating with the MIB1 mutations and LVNC. In experiments with mice harboring the orthologous variants on the corresponding Mib1 backgrounds, triple heterozygous Mib1 Apcdd1 Asxl3 mice showed LVNC, whereas quadruple heterozygous Mib1 Cep192 Tmx3;Bcl7a mice developed bicuspid aortic valve and other valve-associated defects. Biochemical analysis suggested interactions between CEP192, BCL7A, and NOTCH. Gene expression profiling of mutant mouse hearts and human induced pluripotent stem cell-derived cardiomyocytes revealed increased cardiomyocyte proliferation and defective morphological and metabolic maturation.Conclusions: These findings reveal a shared genetic substrate underlying LVNC and bicuspid aortic valve in which MIB1-NOTCH variants plays a crucial role in heterozygous combination with cosegregating genetic modifiers. [ABSTRACT FROM AUTHOR]

Published

2023

12. MINI BODY1, encoding a MATE/DTX family transporter, affects plant architecture in mungbean (Vigna radiata L.).

Author

Xin Li, Yahui Jia, Mingzhu Sun, Zikun Ji, Hui Zhang, Dan Qiu, Qiao Cai, Yan Xia, Xingxing Yuan, Xin Chen, and Zhenguo Shen

Subjects

MUNG bean, GENETIC overexpression, MOLECULAR cloning, POISONS, PLANT development, ESCHERICHIA coli

Abstract

It has been shown that multidrug and toxic compound extrusion/detoxification (MATE/DTX) family transporters are involved in the regulation of plant development and stress response. Here, we characterized the mini body1 (mib1) mutants in mungbean, which gave rise to increased branches, pentafoliate compound leaves, and shortened pods. Map-based cloning revealed that MIB1 encoded a MATE/DTX family protein in mungbean. qRTPCR analysis showed that MIB1 was expressed in all tissues of mungbean, with the highest expression level in the young inflorescence. Complementation assays in Escherichia coli revealed that MIB1 potentially acted as a MATE/DTX transporter in mungbean. It was found that overexpression of the MIB1 gene partially rescued the shortened pod phenotype of the Arabidopsis dtx54 mutant. Transcriptomic analysis of the shoot buds and young pods revealed that the expression levels of several genes involved in the phytohormone pathway and developmental regulators were altered in the mib1 mutants. Our results suggested that MIB1 plays a key role in the control of plant architecture establishment in mungbean. [ABSTRACT FROM AUTHOR]

Published

2022

13. Genome‐wide association study revealed ABCD4 on SSC7 and GREB1L and MIB1 on SSC6 as crucial candidate genes for rib number in Beijing Black pigs.

Author

Niu, Naiqi, Liu, Qian, Hou, Xinhua, Liu, Xin, Wang, Ligang, Zhao, Fuping, Gao, Hongmei, Shi, Lijun, Wang, Lixian, and Zhang, Longchao

Subjects

*GENOME-wide association studies, *LOCUS (Genetics), *ANIMAL variation, *GENES, *SWINE, *SWINE breeding

Abstract

As one of the few animals with variation in the number of rib pairs (RIB), the pig is a good model to study the mechanism of RIB regulation. Quantitative trait loci (QTL) for porcine RIB are present on Sus scrofa chromosome 7 (SSC7). Although several candidate genes exist in this QTL region on SSC7, the causal gene has yet to be verified. Beijing Black pig with 14–17 RIB is a good population for candidate gene mining and 1104 individuals were genotyped using the Illumina Porcine 50K BeadChip. A total of 14 SNPs from 95.49 to 97.78 Mb on SSC7 showed genome‐wide significant association with RIB. On SSC7, a locuszoom plot using pairwise linkage disequilibrium displayed the narrowest linkage region encompassing only two genes, ABCD4 and VRTN. In mice, a transcriptome expression profile was obtained using three embryos at E9.5 (the critical period for rib formation). ABCD4 was highly expressed, but no expression of VRTN was detected. On SSC6, there were four genome‐wide significant SNPs from 106.42 to 106.92 Mb associated with RIB. GREB1L and MIB1, in this region, were regarded as novel candidate genes. These results revealed a crucial candidate causal gene on SSC7 and novel genes on SSC6 for rib number and provided interesting new insights into its genetic basis. [ABSTRACT FROM AUTHOR]

Published

2022

14. Evaluation of the Expression Levels of Notch Signaling Pathway-Related Genes; JAG1, CXCR4, and MIB1 in Acute Myeloid Leukemia Patients.

Author

Ghafelehbashi, Seyedeh Hananeh, Sadeghizadeh, Dina, Rohollah, Fatemeh, Pahlavanneshan, Saghar, and Sadeghizadeh, Majid

Subjects

REVERSE transcriptase polymerase chain reaction, STATISTICS, CELL receptors, CASE-control method, BLOOD collection, MANN Whitney U Test, GENE expression, CELLULAR signal transduction, CANCER patients, CANCER genes, DESCRIPTIVE statistics, TUMOR markers, RECEIVER operating characteristic curves, DATA analysis, DATA analysis software

Abstract

Background: Acute myeloid leukemia (AML) is a complex disease characterized by clonal expansion of undifferentiated myeloid precursors, resulting in impaired hematopoiesis and bone marrow failure. Different genetic and environmental factors are believed to be involved in the pathogenesis of AML. Notch signaling with a tumor suppressing plays a role in myeloproliferative disorder and is a negative regulator of myeloid progenitor commitment. Crosstalk between Notch signaling and CXCR4 axis is a matter of debate in AML. Method: In the current case-control study, we evaluated the expression level of CXCR4, JAG1, and MIB1, which are all involved or related to Notch signaling in adult AML patients. Blood samples were obtained from 25 AML and 17 healthy individuals and the expression level of the selected genes was evaluated via the real-time polymerase chain reaction. Results: Our results revealed the increased expression of JAG1, but decreased expression of CXCR4 in AML patients in Iranian population of AML patients. Moreover, some gender-associated effects on the expression of JAG1 and CXCR4 were detected, which may be related to sex hormones. The expression level of MIB1 did not change significantly. The correlation analysis showed no correlations between the age of the patients and the expression levels of the genes. Conclusion: Herein, for the first time, we suggested some new evidence regarding the complex role of Notch signaling-related genes (CXCR4 and JAG1) in the pathogenesis of AML in Iranian patients. [ABSTRACT FROM AUTHOR]

Published

2022

15. MIB1 upregulates IQGAP1 and promotes pancreatic cancer progression by inducing ST7 degradation

Author

Bin Zhang, Xiang Cheng, Sudong Zhan, Xin Jin, and Tao Liu

Subjects

IQGAP1, MIB1, pancreatic cancer, ST7, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Despite recent progress in cancer treatment, the prognosis of patients with pancreatic cancer still remains poor. Pancreatic tumors are reported to display high molecular heterogeneity. Elucidating the molecular mechanisms underlying pancreatic cancer progression is essential for improving patient treatment and survival. The overexpression of E3 ubiquitin ligase mind bomb 1 (MIB1) was previously described in pancreatic cancer cells, where it enhanced tumor cell proliferation. However, the role of MIB1 in pancreatic cancer progression remains elusive. In the present study, we confirmed that MIB1 expression is elevated in pancreatic cancer tissues and that high levels of MIB associate with unfavorable prognosis. Overexpression of MIB1 enhanced proliferation and invasion of pancreatic cancer cells both in vitro and in vivo. We further investigated the molecular mechanisms downstream of MIB1 and observed for the first time that MIB1 targets suppressor of tumorigenicity 7 protein (ST7), previously described as suppressor of tumorigenicity, for proteasomal degradation. Furthermore, we found that ST7 suppressed tumor growth by downregulating IQ motif containing GTPase activating protein 1 (IQGAP1) in pancreatic tumor cells. Thus, these data show that MIB1 promotes pancreatic cancer progression by inducing ST7 degradation followed by downregulation of IQGAP1 in pancreatic cancer cells. In conclusion, our research shows that the MIB1/ST7/IQGAP1 axis is essential for pancreatic cancer progression, and MIB1 inhibition may serve as a novel therapeutic strategy in patients with pancreatic cancer.

Published

2021

16. A Nucleolar Protein, Nepro, Is Essential for the Maintenance of Early Neural Stem Cells and Preimplantation Embryos

Author

Saito, Tetsuichiro, Crusio, Wim E., Series Editor, Lambris, John D., Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, Reichrath, Jörg, editor, and Reichrath, Sandra, editor

Published

2020

17. Notch signaling is a critical initiator of roof plate formation as revealed by the use of RNA profiling of the dorsal neural tube

Author

Shai Ofek, Sophie Wiszniak, Sarah Kagan, Markus Tondl, Quenten Schwarz, and Chaya Kalcheim

Subjects

BMP, Quail embryos, delta1, Dorsal interneurons, Fate segregation, Mib1, Biology (General), QH301-705.5

Abstract

Abstract Background The dorsal domain of the neural tube is an excellent model to investigate the generation of complexity during embryonic development. It is a highly dynamic and multifaceted region being first transiently populated by prospective neural crest (NC) cells that sequentially emigrate to generate most of the peripheral nervous system. Subsequently, it becomes the definitive roof plate (RP) of the central nervous system. The RP, in turn, constitutes a patterning center for dorsal interneuron development. The factors underlying establishment of the definitive RP and its segregation from NC and dorsal interneurons are currently unknown. Results We performed a transcriptome analysis at trunk levels of quail embryos comparing the dorsal neural tube at premigratory NC and RP stages. This unraveled molecular heterogeneity between NC and RP stages, and within the RP itself. By implementing these genes, we asked whether Notch signaling is involved in RP development. First, we observed that Notch is active at the RP-interneuron interface. Furthermore, gain and loss of Notch function in quail and mouse embryos, respectively, revealed no effect on early NC behavior. Constitutive Notch activation caused a local downregulation of RP markers with a concomitant development of dI1 interneurons, as well as an ectopic upregulation of RP markers in the interneuron domain. Reciprocally, in mice lacking Notch activity, both the RP and dI1 interneurons failed to form and this was associated with expansion of the dI2 population. Conclusions Collectively, our results offer a new resource for defining specific cell types, and provide evidence that Notch is required to establish the definitive RP, and to determine the choice between RP and interneuron fates, but not the segregation of RP from NC.

Published

2021

18. COX2 expression is associated with preoperative tumor volume but not with volumetric tumor growth in vestibular schwannoma

Author

Felix Behling, Elisa Suhm, Vanessa Ries, Vítor Moura Gonçalves, Ghazaleh Tabatabai, Marcos Tatagiba, and Jens Schittenhelm

Subjects

Vestibular schwannoma, Acoustic neuroma, COX2, Tissue microarray, MIB1, Volumetric tumor growth, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Objective Vestibular schwannomas (VS) are benign slow growing tumors arising from the vestibular nerve. The role of cyclooxygenase 2 (COX2) in tumor development of growth has been addressed in a few studies with contradictory results and suggestions. We recently analyzed the immunohistochemical expression of COX2 in 1044 VS samples and described an association of higher COX2 expression with proliferation but found no influence by regular intake of acetylsalicylic acid. We now collected volumetric radiographic data of the preoperative tumor volume and growth to further test the role of COX2 in VS growth. Methods Preoperative images of 898 primary sporadic vestibular schwannomas were assessed, and sufficient preoperative imaging was used for the volumetric measurement preoperative tumor volume (n = 747) and preoperative relative tumor growth (n = 171). Clinical parameters and results of the immunohistochemical expression of COX2 and MIB1 in resected tumor tissue samples were obtained from our prior study. ANOVA, CART-analysis and multivariate nominal logistic regression were used for statistical analysis. Results Larger preoperative tumor volumes were observed with tumors of younger patients (p = 0.0288) and with higher COX2 expression scores (p

Published

2021

19. Proliferative index facilitates distinction between benign biliary lesions and intrahepatic cholangiocarcinoma

Author

Tsokos, Christos G, Krings, Gregor, Yilmaz, Funda, Ferrell, Linda D, and Gill, Ryan M

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Digestive Diseases - (Gallbladder), Cancer, Liver Cancer, Rare Diseases, Liver Disease, Digestive Diseases, Adult, Aged, Aged, 80 and over, Bile Duct Neoplasms, Biliary Tract Diseases, Cell Proliferation, Cholangiocarcinoma, Diagnosis, Differential, Female, Humans, Immunohistochemistry, Ki-67 Antigen, Male, Middle Aged, Predictive Value of Tests, Reproducibility of Results, Tumor Suppressor Protein p53, Bile duct adenoma, Biliary hamartoma, Von Meyenburg complex, Ki-67, Mib1, Pathology, Clinical sciences

Abstract

Differentiation between benign and malignant lesions of the hepatic biliary tree may pose a diagnostic problem because well-differentiated intrahepatic cholangiocarcinoma may mimic biliary hamartoma, bile duct adenoma, or parenchymal extinction. We evaluated Ki-67 proliferative index and p53 status by immunohistochemical staining to aid in exclusion of cholangiocarcinoma. Fourteen biliary hamartomas, 21 bile duct adenomas, and 11 livers with parenchymal extinction were compared with 26 intrahepatic cholangiocarcinomas (16 well-differentiated and 10 moderately or poorly differentiated tumors). We found an increased proliferative index in intrahepatic cholangiocarcinomas compared with benign biliary lesions (average 23.0% in cholangiocarcinoma versus 1.4% in all benign biliary lesions, n = 26 versus n = 46, P < .001). No difference in average proliferative index was observed between well-differentiated and moderately/poorly differentiated cholangiocarcinomas (average 22.7% versus 23.3%, n = 16 versus n = 10, P = .92). Average proliferation indices of benign biliary lesions were uniformly low (biliary hamartoma, 1.2%; bile duct adenoma, 2%; parenchymal extinction, 0.5%). Most cholangiocarcinomas (23/26; 88.5%), but none of the benign lesions (0/46; 0%), had proliferative indices greater than 10%. Strong nuclear p53 immunohistochemical staining was only seen in cholangiocarcinomas (9/26; 34.6%) and not in benign biliary lesions (0/46; 0%), although many of the benign lesions showed weak to moderate staining. Immunohistochemical staining for Ki-67 facilitates distinction between benign and malignant lesions of the intrahepatic biliary tree, whereas p53 immunohistochemical staining is less helpful.

Published

2016

20. A novel peptide encoded by N6-methyladenosine modified circMAP3K4 prevents apoptosis in hepatocellular carcinoma.

Author

Duan, Jin-Ling, Chen, Wei, Xie, Juan-Juan, Zhang, Mao-Lei, Nie, Run-Cong, Liang, Hu, Mei, Jie, Han, Kai, Xiang, Zhi-Cheng, Wang, Feng-Wei, Teng, Kai, Chen, Ri-Xin, Deng, Min-Hua, Yin, Yi-Xin, Zhang, Nu, Xie, Dan, and Cai, Mu-Yan

Subjects

PEPTIDES, HEPATOCELLULAR carcinoma, ADENOSINES, PROGRESSION-free survival, UBIQUITIN ligases, CISPLATIN

Abstract

Background: Circular RNAs (circRNAs) regulate various biological activities and have been shown to play crucial roles in hepatocellular carcinoma (HCC) progression. However, only a few coding circRNAs have been identified in cancers, and their roles in HCC remain elusive. This study aimed to identify coding circRNAs and explore their function in HCC. Methods: CircMAP3K4 was selected from the CIRCpedia database. We performed a series of experiments to determine the characteristics and coding capacity of circMAP3K4. We then used in vivo and in vitro assays to investigate the biological function and mechanism of circMAP3K4 and its protein product, circMAP3K4-455aa, in HCC. Results: We found circMAP3K4 to be an upregulated circRNA with coding potential in HCC. IGF2BP1 recognized the circMAP3K4 N6-methyladenosine modification and promoted its translation into circMAP3K4-455aa. Functionally, circMAP3K4-455aa prevented cisplatin-induced apoptosis in HCC cells by interacting with AIF, thus protecting AIF from cleavage and decreasing its nuclear distribution. Moreover, circMAP3K4-455aa was degraded through the ubiquitin–proteasome E3 ligase MIB1 pathway. Clinically, a high level of circMAP3K4 is an independent prognostic factor for adverse overall survival and adverse disease-free survival of HCC patients. Conclusions: CircMAP3K4 is a highly expressed circRNA in HCC. Driven by m6A modification, circMAP3K4 encoded circMAP3K4-455aa, protected HCC cells from cisplatin exposure, and predicted worse prognosis of HCC patients. Targeting circMAP3K4-455aa may provide a new therapeutic strategy for HCC patients, especially for those with chemoresistance. CircMAP3K4 is a highly expressed circRNA in HCC. Driven by m6A modification, IGF2BP1 facilitates circMAP3K4 peptide translation, then the circMAP3K4 peptide inhibits AIF cleavage and nuclear distribution, preventing HCC cells from cell death under stress and promoting HCC progression. [ABSTRACT FROM AUTHOR]

Published

2022

21. A Novel Long-Noncoding RNA LncZFAS1 Prevents MPP+-Induced Neuroinflammation Through MIB1 Activation.

Author

Zhu, Ziman, Huang, Peiling, Sun, Ruifeng, Li, Xiaoling, Li, Wenshan, and Gong, Weijun

Abstract

Parkinson's disease remains one of the leading neurodegenerative diseases in developed countries. Despite well-defined symptomology and pathology, the complexity of Parkinson's disease prevents a full understanding of its etiological mechanism. Mechanistically, α-synuclein misfolding and aggregation appear to be central for disease progression, but mitochondrial dysfunction, dysfunctional protein clearance and ubiquitin/proteasome systems, and neuroinflammation have also been associated with Parkinson's disease. Particularly, neuroinflammation, which was initially thought to be a side effect of Parkinson's disease pathogenesis, has now been recognized as driver of Parkinson's disease exacerbation. Next-generation sequencing has been used to identify a plethora of long noncoding RNAs (lncRNA) with important transcriptional regulatory functions. Moreover, a myriad of lncRNAs are known to be regulators of inflammatory signaling and neurodegenerative diseases, including IL-1β secretion and Parkinson's disease. Here, LncZFAS1 was identified as a regulator of inflammasome activation, and pyroptosis in human neuroblast SH-SY5Y cells following MPP+ treatment, a common in vitro Parkinson's disease cell model. Mechanistically, TXNIP ubiquitination through MIB1 E3 ubiquitin ligase regulates NLRP3 inflammasome activation in neuroblasts. In contrast, MPP+ activates the NLPR3 inflammasome through miR590-3p upregulation and direct interference with MIB1-dependent TXNIP ubiquitination. LncZFAS overexpression inhibits this entire pathway through direct interference with miR590-3p, exposing a novel research idea regarding the mechanism of Parkinson's disease. [ABSTRACT FROM AUTHOR]

Published

2022

22. Increased proliferation is associated with CNS invasion in meningiomas.

Author

Behling, Felix, Fodi, Christina, Wang, Sophie, Hempel, Johann-Martin, Hoffmann, Elgin, Tabatabai, Ghazaleh, Honegger, Jürgen, Tatagiba, Marcos, Schittenhelm, Jens, and Skardelly, Marco

Abstract

Introduction: Meningiomas are the most common benign intracranial neoplasms. CNS invasion in meningiomas has been integrated into the 2016 WHO classification of CNS tumors as a stand-alone criterion for atypia. Since then, its prognostic impact has been debated based on contradictory results from retrospective analyses. The aim of the study was to elucidate whether histopathological evidence of CNS invasion is associated with increased proliferative potential. Methods: We have conducted a quantified measurement of the proliferation marker Ki67 and analyzed its association with CNS invasion determined by histology together with other established prognostic markers of progression. Routine, immunohistochemical staining for Ki67 were digitalized and automatic quantification was done using Image J software. Results: Overall, 1718 meningiomas were assessed. Histopathological CNS invasion was seen in 108 cases (6.7%). Uni- and multivariate analysis revealed a significantly higher Ki67 proliferation rate in meningiomas with CNS invasion (p < 0.0001 and p = 0.0098, respectively). Conclusions: Meningiomas with histopathological CNS invasion show a higher proliferative activity. [ABSTRACT FROM AUTHOR]

Published

2021

23. MIB1 upregulates IQGAP1 and promotes pancreatic cancer progression by inducing ST7 degradation.

Author

Zhang, Bin, Cheng, Xiang, Zhan, Sudong, Jin, Xin, and Liu, Tao

Abstract

Despite recent progress in cancer treatment, the prognosis of patients with pancreatic cancer still remains poor. Pancreatic tumors are reported to display high molecular heterogeneity. Elucidating the molecular mechanisms underlying pancreatic cancer progression is essential for improving patient treatment and survival. The overexpression of E3 ubiquitin ligase mind bomb 1 (MIB1) was previously described in pancreatic cancer cells, where it enhanced tumor cell proliferation. However, the role of MIB1 in pancreatic cancer progression remains elusive. In the present study, we confirmed that MIB1 expression is elevated in pancreatic cancer tissues and that high levels of MIB associate with unfavorable prognosis. Overexpression of MIB1 enhanced proliferation and invasion of pancreatic cancer cells both in vitro and in vivo. We further investigated the molecular mechanisms downstream of MIB1 and observed for the first time that MIB1 targets suppressor of tumorigenicity 7 protein (ST7), previously described as suppressor of tumorigenicity, for proteasomal degradation. Furthermore, we found that ST7 suppressed tumor growth by downregulating IQ motif containing GTPase activating protein 1 (IQGAP1) in pancreatic tumor cells. Thus, these data show that MIB1 promotes pancreatic cancer progression by inducing ST7 degradation followed by downregulation of IQGAP1 in pancreatic cancer cells. In conclusion, our research shows that the MIB1/ST7/IQGAP1 axis is essential for pancreatic cancer progression, and MIB1 inhibition may serve as a novel therapeutic strategy in patients with pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2021

24. Notch signalling defines dorsal root ganglia neuroglial fate choice during early neural crest cell migration

Author

Sophie Wiszniak and Quenten Schwarz

Subjects

Notch signalling, Mib1, Neural crest, Fate restriction, Dorsal root ganglia, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurophysiology and neuropsychology, QP351-495

Abstract

Abstract Background The dorsal root ganglia (DRG) are a critical component of the peripheral nervous system, and function to relay somatosensory information from the body’s periphery to sensory perception centres within the brain. The DRG are primarily comprised of two cell types, sensory neurons and glia, both of which are neural crest-derived. Notch signalling is known to play an essential role in defining the neuronal or glial fate of bipotent neural crest progenitors that migrate from the dorsal ridge of the neural tube to the sites of the DRG. However, the involvement of Notch ligands in this process and the timing at which neuronal versus glial fate is acquired has remained uncertain. Results We have used tissue specific knockout of the E3 ubiquitin ligase mindbomb1 (Mib1) to remove the function of all Notch ligands in neural crest cells. Wnt1-Cre; Mib1 fl/fl mice exhibit severe DRG defects, including a reduction in glial cells, and neuronal cell death later in development. By comparing formation of sensory neurons and glia with the expression and activation of Notch signalling in these mice, we define a critical period during embryonic development in which early migrating neural crest cells become biased toward neuronal and glial phenotypes. Conclusions We demonstrate active Notch signalling between neural crest progenitors as soon as trunk neural crest cells delaminate from the neural tube and during their early migration toward the site of the DRG. This data brings into question the timing of neuroglial fate specification in the DRG and suggest that it may occur much earlier than originally considered.

Published

2019

25. Notch signaling is a critical initiator of roof plate formation as revealed by the use of RNA profiling of the dorsal neural tube.

Author

Ofek, Shai, Wiszniak, Sophie, Kagan, Sarah, Tondl, Markus, Schwarz, Quenten, and Kalcheim, Chaya

Subjects

NEURAL tube, NEURAL crest, PERIPHERAL nervous system, NOTCH genes, EMBRYOLOGY, CENTRAL nervous system

Abstract

Background: The dorsal domain of the neural tube is an excellent model to investigate the generation of complexity during embryonic development. It is a highly dynamic and multifaceted region being first transiently populated by prospective neural crest (NC) cells that sequentially emigrate to generate most of the peripheral nervous system. Subsequently, it becomes the definitive roof plate (RP) of the central nervous system. The RP, in turn, constitutes a patterning center for dorsal interneuron development. The factors underlying establishment of the definitive RP and its segregation from NC and dorsal interneurons are currently unknown. Results: We performed a transcriptome analysis at trunk levels of quail embryos comparing the dorsal neural tube at premigratory NC and RP stages. This unraveled molecular heterogeneity between NC and RP stages, and within the RP itself. By implementing these genes, we asked whether Notch signaling is involved in RP development. First, we observed that Notch is active at the RP-interneuron interface. Furthermore, gain and loss of Notch function in quail and mouse embryos, respectively, revealed no effect on early NC behavior. Constitutive Notch activation caused a local downregulation of RP markers with a concomitant development of dI1 interneurons, as well as an ectopic upregulation of RP markers in the interneuron domain. Reciprocally, in mice lacking Notch activity, both the RP and dI1 interneurons failed to form and this was associated with expansion of the dI2 population. Conclusions: Collectively, our results offer a new resource for defining specific cell types, and provide evidence that Notch is required to establish the definitive RP, and to determine the choice between RP and interneuron fates, but not the segregation of RP from NC. [ABSTRACT FROM AUTHOR]

Published

2021

26. Left Ventricular Myocardial Noncompaction with Advanced Atrioventricular Conduction Disorder and Ventricular Arrhythmias in a Young Patient: Role of MIB1 Gene

Author

Cristina Balla, Martina De Raffele, Maria Angela Deserio, Mariabeatrice Sanchini, Marianna Farnè, Cecilia Trabanelli, Luca Ragni, Mauro Biffi, Alessandra Ferlini, Claudio Rapezzi, Francesca Gualandi, and Matteo Bertini

Subjects

left ventricular noncompaction, advanced atrioventricular block, MIB1, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Left ventricular noncompaction (LVNC) is a structural abnormality of the left ventricle, usually described as an isolated condition, or sometimes associated with other structural cardiac diseases. LVNC is generally asymptomatic, although it may present conduction disorders, arrhythmias, and heart failure. Here, we present the case of a patient who came to our attention with a severe LVNC phenotype associated with advanced AV conduction disorder, and supraventricular and ventricular arrhythmias at young age, in which a novel MIB1, likely pathogenic, variation has been identified.

Published

2021

27. A Human Hereditary Cardiomyopathy Shares a Genetic Substrate with Bicuspid Aortic Valve:[Inkl. Correction]

Author

Siguero-Álvarez, Marcos, Salguero-Jiménez, Alejandro, Grego-Bessa, Joaquim, De La Barrera, Jorge, MacGrogan, Donal, Prados, Belén, Sánchez-Sáez, Fernando, Piñeiro-Sabarís, Rebeca, Felipe-Medina, Natalia, Torroja, Carlos, Gómez, Manuel José, Sabater-Molina, María, Escribá, Rubén, Richaud-Patin, Ivonne, Iglesias-García, Olalla, Sbroggio, Mauro, Callejas, Sergio, O'Regan, Declan P., McGurk, Kathryn A., Dopazo, Ana, Giovinazzo, Giovanna, Ibañez, Borja, Monserrat, Lorenzo, Pérez-Pomares, José María, Sánchez-Cabo, Fátima, Pendas, Alberto M., Raya, Angel, Gimeno-Blanes, Juan R., De La Pompa, José Luis, Siguero-Álvarez, Marcos, Salguero-Jiménez, Alejandro, Grego-Bessa, Joaquim, De La Barrera, Jorge, MacGrogan, Donal, Prados, Belén, Sánchez-Sáez, Fernando, Piñeiro-Sabarís, Rebeca, Felipe-Medina, Natalia, Torroja, Carlos, Gómez, Manuel José, Sabater-Molina, María, Escribá, Rubén, Richaud-Patin, Ivonne, Iglesias-García, Olalla, Sbroggio, Mauro, Callejas, Sergio, O'Regan, Declan P., McGurk, Kathryn A., Dopazo, Ana, Giovinazzo, Giovanna, Ibañez, Borja, Monserrat, Lorenzo, Pérez-Pomares, José María, Sánchez-Cabo, Fátima, Pendas, Alberto M., Raya, Angel, Gimeno-Blanes, Juan R., and De La Pompa, José Luis

Abstract

Background: The complex genetics underlying human cardiac disease is evidenced by its heterogenous manifestation, multigenic basis, and sporadic occurrence. These features have hampered disease modeling and mechanistic understanding. Here, we show that 2 structural cardiac diseases, left ventricular noncompaction (LVNC) and bicuspid aortic valve, can be caused by a set of inherited heterozygous gene mutations affecting the NOTCH ligand regulator MIB1 (MINDBOMB1) and cosegregating genes. Methods: We used CRISPR-Cas9 gene editing to generate mice harboring a nonsense or a missense MIB1 mutation that are both found in LVNC families. We also generated mice separately carrying these MIB1 mutations plus 5 additional cosegregating variants in the ASXL3, APCDD1, TMX3, CEP192, and BCL7A genes identified in these LVNC families by whole exome sequencing. Histological, developmental, and functional analyses of these mouse models were carried out by echocardiography and cardiac magnetic resonance imaging, together with gene expression profiling by RNA sequencing of both selected engineered mouse models and human induced pluripotent stem cell-derived cardiomyocytes. Potential biochemical interactions were assayed in vitro by coimmunoprecipitation and Western blot. Results: Mice homozygous for the MIB1 nonsense mutation did not survive, and the mutation caused LVNC only in heteroallelic combination with a conditional allele inactivated in the myocardium. The heterozygous MIB1 missense allele leads to bicuspid aortic valve in a NOTCH-sensitized genetic background. These data suggest that development of LVNC is influenced by genetic modifiers present in affected families, whereas valve defects are highly sensitive to NOTCH haploinsufficiency. Whole exome sequencing of LVNC families revealed single-nucleotide gene variants of ASXL3, APCDD1, TMX3, CEP192, and BCL7A cosegregating with the MIB1 mutations and LVNC. In experiments with mice harboring the orthologous variants on the cor

Published

2023

28. A Novel Long-Noncoding RNA LncZFAS1 Prevents MPP+-Induced Neuroinflammation Through MIB1 Activation

Author

Zhu, Ziman, Huang, Peiling, Sun, Ruifeng, Li, Xiaoling, Li, Wenshan, and Gong, Weijun

Published

2022

29. CytoLyt fixation significantly inhibits MIB1 immunoreactivity whereas alternative Ki‐67 clone 30‐9 is not susceptible to the inhibition: Critical diagnostic implications.

Author

Buonocore, Darren J., Konno, Fumiko, Jungbluth, Achim A., Frosina, Denise, Fayad, Mariam, Edelweiss, Marcia, Lin, Oscar, and Rekhtman, Natasha

Abstract

Background: The Ki‐67 proliferation marker has multiple diagnostic and prognostic applications. Although several clones to the Ki‐67 antigen are commercially available, the MIB1 clone is widely recommended in the surgical pathology literature for neuroendocrine tumors. In our cytopathology practice, we have encountered unexpectedly low MIB1 immunoreactivity in CytoLyt‐fixed cell blocks (CBs). The current study evaluated the impact of fixatives, CB processing, and immunocytochemical (ICC) procedures on Ki‐67 immunoreactivity. Methods: Test CBs were prepared from freshly resected tumors, and multiple variables in the MIB1 ICC procedure were tested, including CytoLyt versus formalin collection media, MIB1 versus other Ki‐67 clones including 30‐9, and other variables. MIB1 versus Ki‐67 30‐9 clones were tested in parallel on CytoLyt‐fixed CBs from clinical samples of small cell lung carcinoma (SCLC). Results: In the test CBs (n = 10), the mean MIB1 labeling index was 10% in CytoLyt versus 47% in formalin (P = .0116), with a mean loss of reactivity in matched CBs of 37% (up to 70%). None of the procedure modifications tested in 223 individual ICC reactions recovered MIB1 reactivity in CytoLyt except for switching to the Ki‐67 30‐9 antibody. In CytoLyt‐fixed SCLC samples (n = 14), the Ki‐67 30‐9 antibody demonstrated expected ranges of reactivity (mean, 83%; range, 60%‐100%), whereas MIB1 demonstrated markedly inhibited labeling (mean, 60%; range, 10%‐95%) (P = .0058). Conclusions: CytoLyt fixation substantially inhibits MIB1 immunoreactivity, whereas the Ki‐67 30‐9 clone is not susceptible to inhibition. Markedly discrepant MIB1 reactivity may present a pitfall in the diagnosis of SCLC and may lead to the incorrect prognostic stratification of other tumor types. For laboratories using CytoLyt, we recommend using the Ki‐67 30‐9 antibody rather than the MIB1 antibody. CytoLyt fixation substantially inhibits MIB1 immunoreactivity and may present a diagnostic pitfall in certain tumors, especially small cell carcinoma. The Ki‐67 30‐9 clone demonstrates adequate performance and should be the clone of choice in laboratories using CytoLyt collection media. [ABSTRACT FROM AUTHOR]

Published

2019

30. Cut‐point for Ki‐67 proliferation index as a prognostic marker for glioblastoma.

Author

Wong, Eugene, Nahar, Najmun, Hau, Eric, Varikatt, Winny, Gebski, Val, Ng, Thomas, Jayamohan, Jayasingham, and Sundaresan, Puma

Subjects

*GLIOBLASTOMA multiforme, *CELL proliferation, *CELL division, *CANCER chemotherapy, *IMMUNOHISTOCHEMISTRY

Abstract

Introduction: Ki‐67 proliferation index (Ki‐67 index) is used to quantify cell proliferation during histopathological assessment of various tumors including glioblastoma (GB). Aim: We aimed to assess correlation between Ki‐67 index and overall survival in patients with GB and determine a cut‐point for Ki‐67 index that predicts for poorer survival. Method: Records of adult patients diagnosed with GB on histopathological specimens at a tertiary cancer center in Sydney between 1 January 2002 and 30 July 2012 were retrieved. Specimens of these patients were examined for quantification of Ki‐67 staining by two independent pathologists. Patient, disease, treatment, and survival data were collected from hospital and cancer care service records. Statistical analysis was performed using proportional hazards models, Kaplan–Meier curves, and the minimum P‐value approach. Result: Of the eligible 71 patients, 58% were males with median age of 58 (range 18–87). Seventy‐three percent of patients were of ECOG performance status 0–1. There was a statistically significant correlation between Ki‐67 index and overall survival. In patients with Ki‐67 > 22% (n = 36), 5‐year survival was approximately 30% compared to 5% in those with Ki‐67 ≤ 22% (n = 35; log‐rank P‐value = 0.04; hazard ratio (HR) = 0.53; 95% confidence intervals (CI), 0.29–0.97). Conclusion: This study demonstrates a positive correlation between Ki‐67 index and overall survival in patients with GB. Percentage staining of Ki‐67 < 22% appears to predict for poorer survival in GB. [ABSTRACT FROM AUTHOR]

Published

2019

31. SNX17 Recruits USP9X to Antagonize MIB1-Mediated Ubiquitination and Degradation of PCM1 during Serum-Starvation-Induced Ciliogenesis

Author

Pengtao Wang, Jianhong Xia, Leilei Zhang, Shaoyang Zhao, Shengbiao Li, Haiyun Wang, Shan Cheng, Heying Li, Wenguang Yin, Duanqing Pei, and Xiaodong Shu

Subjects

snx17, usp9x, pcm1, mib1, centriolar satellite, cilia, Cytology, QH573-671

Abstract

Centriolar satellites are non-membrane cytoplasmic granules that deliver proteins to centrosome during centrosome biogenesis and ciliogenesis. Centriolar satellites are highly dynamic during cell cycle or ciliogenesis and how they are regulated remains largely unknown. We report here that sorting nexin 17 (SNX17) regulates the homeostasis of a subset of centriolar satellite proteins including PCM1, CEP131, and OFD1 during serum-starvation-induced ciliogenesis. Mechanistically, SNX17 recruits the deubiquitinating enzyme USP9X to antagonize the mindbomb 1 (MIB1)-induced ubiquitination and degradation of PCM1. SNX17 deficiency leads to enhanced degradation of USP9X as well as PCM1 and disrupts ciliogenesis upon serum starvation. On the other hand, SNX17 is dispensable for the homeostasis of PCM1 and USP9X in serum-containing media. These findings reveal a SNX17/USP9X mediated pathway essential for the homeostasis of centriolar satellites under serum starvation, and provide insight into the mechanism of USP9X in ciliogenesis, which may lead to a better understating of USP9X-deficiency-related human diseases such as X-linked mental retardation and neurodegenerative diseases.

Published

2019

32. Mib1 contributes to persistent directional cell migration by regulating the Ctnnd1-Rac1 pathway.

Author

Takamasa Mizoguchi, Shoko Ikeda, Saori Watanabe, Michiko Sugawara, and Motoyuki Itoh

Subjects

*CELL migration, *CATENINS, *UBIQUITIN ligases, *RAS oncogenes, *F-actin, *GUANOSINE triphosphatase, *UBIQUITINATION, *CELLULAR signal transduction

Abstract

Persistent directional cell migration is involved in animal development and diseases. The small GTPase Rac1 is involved in F-actin and focal adhesion dynamics. Local Rac1 activity is required for persistent directional migration, whereas global, hyperactivated Rac1 enhances random cell migration. Therefore, precise control of Rac1 activity is important for proper directional cell migration. However, the molecular mechanism underlying the regulation of Rac1 activity in persistent directional cell migration is not fully understood. Here, we show that the ubiquitin ligase mind bomb 1 (Mib1) is involved in persistent directional cell migration. We found that knockdown of MIB1 led to an increase in random cell migration in HeLa cells in a wound-closure assay. Furthermore, we explored novel Mib1 substrates for cell migration and found that Mib1 ubiquitinates Ctnnd1. Mib1-mediated ubiquitination of Ctnnd1 K547 attenuated Rac1 activation in cultured cells. In addition, we found that posterior lateral line primordium cells in the zebrafish mib1ta52b mutant showed increased random migration and loss of directional F-actin-based protrusion formation. Knockdown of Ctnnd1 partially rescued posterior lateral line primordium cell migration defects in the mib1ta52b mutant. Taken together, our data suggest that Mib1 plays an important role in cell migration and that persistent directional cell migration is regulated, at least in part, by the Mib1-Ctnnd1-Rac1 pathway. [ABSTRACT FROM AUTHOR]

Published

2017

33. The Retinal Pigment Epithelium Is a Notch Signaling Niche in the Mouse Retina.

Author

Ha, Taejeong, Moon, Kyeong Hwan, Dai, Le, Hatakeyama, Jun, Yoon, Keejung, Park, Hee-Sae, Kong, Young-Yoon, Shimamura, Kenji, and Kim, Jin Woo

Abstract

Summary Notch signaling in neural progenitor cell is triggered by ligands expressed in adjacent cells. To identify the sources of active Notch ligands in the mouse retina, we negatively regulated Notch ligand activity in various neighbors of retinal progenitor cells (RPCs) by eliminating mindbomb E3 ubiquitin protein ligase 1 (Mib1). Mib1-deficient retinal cells failed to induce Notch activation in intra-lineage RPCs, which prematurely differentiated into neurons; however, Mib1 in post-mitotic retinal ganglion cells was not important. Interestingly, Mib1 in the retinal pigment epithelium (RPE) also contributed to Notch activation in adjacent RPCs by supporting the localization of active Notch ligands at RPE-RPC contacts. Combining this RPE-driven Notch signaling and intra-retinal Notch signaling, we propose a model in which one RPC daughter receives extra Notch signals from the RPE to become an RPC, whereas its sister cell receives only a subthreshold level of intra-retinal Notch signal and differentiates into a neuron. [ABSTRACT FROM AUTHOR]

Published

2017

34. Comparison between Ki67 labeling index determined using image analysis software with virtual slide system and that determined visually in breast cancer.

Author

Maeda, Ichiro, Abe, Kayoko, Koizumi, Hirotaka, Nakajima, Chika, Tajima, Shinya, Aoki, Hiromi, Tsuchiya, Junichi, Tsuchiya, Seiko, Tsuchiya, Kyoko, Shimo, Arata, Tsugawa, Koichiro, Ueno, Takahiko, Tatsunami, Shinobu, and Takagi, Masayuki

Abstract

Background: In recent papers, Ki67 labeling index (LI) has been used to classify breast cancer patients into the low and high Ki67LI groups for comparison studies, which showed significant differences in many prognostic factors. It has not been clarified whether image analysis software can be used for calculating LI in breast cancer. In our study, we examined whether Ki67LI in breast cancer calculated using image analysis software correlates with that measured on the basis of visual. Methods: Fifty patients were randomly selected among breast cancer patients who underwent surgical operation from March, 2010 to May, 2010 in our hospital without preoperative chemotherapy. In this study, for the virtual slide system (VSS: VS120-L100, Olympus, Tokyo, Japan), the high-resolution VSs of all the 50 patients were prepared as samples. The image analysis software use for calculating LI was Tissuemorph Digital Pathology (Tissuemorph DP: Visiopharm, Hoersholm, Denmark). The calculated LI was extracted from 3 to 5 views containing hot spots. The LI calculated using Tissuemorph DP was designed as LI/image/T. The digital image of 3 to 5 LI/image/T views was printed out, and on the digital photograph, we counted visually the number of Ki67-immunopositive cells in exactly the same area, and the percentage of Ki67-immunopositive cells was designed as LI/direct. Moreover, a pathologist's assistant (PA) determined the tumor area in the same specimen using VSS and calculated LI using Tissuemorph DP, which was designed as LI/image/PA. The chief pathologist (CP) similarly calculated LI which was designed as LI/image/CP. We evaluated the degree of agreement between different data sets 'LI/image/T and LI/direct' and 'LI/image/T, LI/image/CP, and LI/image/PA' by using interclass correlation coefficient (ICC). Results: The average counts of cells were as follows: LI/direct, 3209.7 ± 1970.4 (SD); LI/image/T, 2601.6 ± 1697.1; LI/image/PA, 2886.5 ± 2027.5; LI/image/CP, 18805.5 ± 22293.4. The values of LI/direct and LI/image/T showed almost perfect agreement as showed by an ICC of 0.885 (95 % CI, 0.806-0.933; p < 0.001). The agreement among three investigators was almost perfect. The obtained ICC was 0.825 (95 % CI, 0.739-0.890; p < 0.001) among the data of LI/image/T, LI/image/CP and LI/image/PA. There were five cases that immunopositivity for Ki67 showed a more than 10 % disagreement between LI/direct and LI/image/T. Conclusion: The merits of calculating Ki67 LI using Tissuemorph DP are as follows. First, the staining intensity of the cells to be counted can be adjusted. Second, the portion of a tumor including 'hot spots' for counting can be chosen. Third, many cancer cells can be counted more rapidly using Tissuemorph DP than by visual observation. However, it is important that pathologist should check and carry out the final decision of the data, when Ki67 LI using Tissuemorph DP is calculated. [ABSTRACT FROM AUTHOR]

Published

2016

35. MicroRNA-10a/10b represses a novel target gene mib1 to regulate angiogenesis.

Author

Xin Wang, Chang Chun Ling, Liping Li, Yinyin Qin, Jialing Qi, Xiaoyu Liu, Bo You, Yunwei Shi, Jie Zhang, Qiu Jiang, Hui Xu, Cheng Sun, Yiwen You, Renjie Chai, and Dong Liu

Subjects

*MICRORNA, *NEOVASCULARIZATION, *PROTEIN-tyrosine kinases, *PHENOTYPES, *ZEBRA danio

Abstract

Aims: MicroRNA-10 (miR-10) was originally shown to regulate angiogenesis by directly modulating the levels of membranebound fms-related tyrosine kinase 1 (mflt1) and its soluble splice isoform sflt1 post-transcriptionally in zebrafish. Given that flt1 knockdown incompletely rescues the angiogenic phenotypes in miR-10 morphants, flt1 is unlikely to be the only important target of miR-10 in endothelial cells (ECs). It will be interesting to investigate new mechanism responsible for angiogenic defect induced by miR-10 knockdown. Methods and results: Firstly, we demonstrated that miR-10a and miR-10b (miR-10a/10b) were highly enriched in embryonic zebrafish ECs using deep sequencing, Taqman polymerase chain reaction, and in situ hybridisation. Subsequently, we proved that loss of miR-10a/10b impaired blood vessel outgrowth through regulating tip cell behaviours. Mib1 was identified as a potential direct target of miR-10a/10b through in silicon analysis and in vitro luciferase sensor assay. In vivo reporter assay in zebrafish embryos confirmed the binding of miR-10 with 3'-UTR of zebrafish mib1. Furthermore, inhibition of mib1 and Notch signaling rescued the angiogenic defects in miR-10-deficient zebrafish embryos. In addition, we provided evidences that miR-10 regulates human ECs behaviour through targeting Mib1 as well. Conclusion: Taken together, these results indicate that miR-10 regulates the angiogenic behaviour in a Notch-dependent manner by directly targeting mib1. [ABSTRACT FROM AUTHOR]

Published

2016

36. Phenotyping Zebrafish Mutant Models to Assess Candidate Genes Associated with Aortic Aneurysm

Author

Andrew Prendergast, Bulat A. Ziganshin, Dimitra Papanikolaou, Mohammad A. Zafar, Stefania Nicoli, Sandip Mukherjee, and John A. Elefteriades

Subjects

Embryo, Nonmammalian, MIB1, variant of unknown significance, VUS, whole exome sequencing, thoracic aortic aneurysm, zebrafish, EMILIN1, Aortic Aneurysm, Thoracic, Pilot Projects, QH426-470, Zebrafish Proteins, Article, Disease Models, Animal, Phenotype, Loss of Function Mutation, Genetics, Animals, Humans, Genetics (clinical)

Abstract

(1) Background: Whole Exome Sequencing of patients with thoracic aortic aneurysm often identifies “Variants of Uncertain Significance” (VUS), leading to uncertainty in clinical management. We assess a novel mechanism for potential routine assessment of these genes in TAA patients. Zebrafish are increasingly used as experimental models of disease. Advantages include low cost, rapid maturation, and physical transparency, permitting direct microscopic assessment. (2) Methods: Zebrafish loss of function mutations were generated using a CRISPRC/CAS9 approach for EMILIN1 and MIB1 genes similar to VUSs identified in clinical testing. Additionally, “positive control” mutants were constructed for known deleterious variants in FBN1 (Marfan’s) and COL1A2, COL5A1, COL5A2 (Ehlers-Danlos). Zebrafish embryos were followed to six days post-fertilization. Embryos were studied by brightfield and confocal microscopy to ascertain any vascular, cardiac, and skeletal abnormalities. (3) Results: A dramatic pattern of cardiac, cerebral, aortic, and skeletal abnormalities was identified for the known pathogenic FBN1 and COL1A2, COL5A1, and COL5A2 mutants, as well as for the EMILIN1 and MIB1 mutants of prior unknown significance. Visualized abnormalities included hemorrhage (peri-aortic and cranial), cardiomegaly, reduced diameter of the aorta and intersegmental vessels, lower aortic cell counts, and scoliosis (often extremely severe). (4) Conclusion: This pilot study suggests that candidate genes arising in clinical practice may be rapidly assessed via zebrafish mutants—thus permitting evidence-based decisions about pathogenicity. Thus, years-long delays to clinically demonstrate pathogenicity may be obviated. Zebrafish data would represent only one segment of analysis, which would also include frequency of the variant in the general population, in silico genetic analysis, and degree of preservation in phylogeny.

Published

2021

37. Left Ventricular Myocardial Noncompaction with Advanced Atrioventricular Conduction Disorder and Ventricular Arrhythmias in a Young Patient: Role of MIB1 Gene

Author

Francesca Gualandi, Martina De Raffele, Cecilia Trabanelli, Cristina Balla, Mariabeatrice Sanchini, Alessandra Ferlini, Claudio Rapezzi, Marianna Farnè, Matteo Bertini, Maria Angela Deserio, Mauro Biffi, and Luca Ragni

Subjects

medicine.medical_specialty, Case Report, Asymptomatic, NO, advanced atrioventricular block, Internal medicine, medicine, Diseases of the circulatory (Cardiovascular) system, Pharmacology (medical), cardiovascular diseases, General Pharmacology, Toxicology and Pharmaceutics, Likely pathogenic, MIB1, business.industry, medicine.disease, Atrioventricular conduction disorder, Young age, Advanced atrioventricular block, MIB1, Left ventricular noncompaction, medicine.anatomical_structure, Ventricle, Heart failure, RC666-701, Cardiology, cardiovascular system, Left ventricular noncompaction, left ventricular noncompaction, Abnormality, medicine.symptom, business

Abstract

Left ventricular noncompaction (LVNC) is a structural abnormality of the left ventricle, usually described as an isolated condition, or sometimes associated with other structural cardiac diseases. LVNC is generally asymptomatic, although it may present conduction disorders, arrhythmias, and heart failure. Here, we present the case of a patient who came to our attention with a severe LVNC phenotype associated with advanced AV conduction disorder, and supraventricular and ventricular arrhythmias at young age, in which a novel MIB1, likely pathogenic, variation has been identified.

Published

2021

38. Medulloblastoma: evaluation of proliferative index by monoclonal antibody Mib-1, its prognostic correlation and therapeutic implications Meduloblastoma: avaliação do padrão proliferativo pelo anticorpo monoclonal Mib-1, correlação prognóstica e implicações terapêuticas

Author

Antonio Fernandes Ferrari, Maria Betânia Mahler Araújo, Paulo Henrique Aguiar, and José Pindaro Pereira Plese

Subjects

meduloblastoma, índice proliferativo (IP), Mib1, fatores prognósticos, medulloblastoma, labelling index (LI), mib-1, prognostic factors, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

In the past few years, the monoclonal antibody MIB-1 has been used by researchers in order to retrospectively study paraffin imbibed tumor fragments. The medulloblastoma is the most common malignant central nervous system tumor in childhood. The objectives were: determination of the mean Mib-1 LI value from these patients, as well as the prognostic value of the method.This retrospective study represents an analysis of the cellular proliferation index of posterior fossa medulloblastomas collected from 22 patients at A.C. Camargo Hospital, from January 1990 to December 1999. The histopathological diagnosis was confirmed by H&E and proliferative index (LI) was achived with Mib-1 which detects proliferating cells during G1, G2, S and M phases.The results demostrated that the mean Mib-1 was 30,1%, and ranged from 5,2% to 62,0%.In conclusion, this method has prognostic value, has to be used as routine for patients harboring medulloblastomas and the ones who have PI greater than the mean value found in this study, should be treated aggressively.Nos últimos anos, o anticorpo monoclonal Mib1 tem sido bastante utilizado pelos pesquisadores para estudo retro e prospectivo, pela possibilidade de se obter um índice de proliferação de fragmentos tumorais conservados em parafina. O meduloblastoma é o tumor maligno mais freqüente do sistema nervoso central na infância. Os objetivos do trabalho foram determinar a média IP através do Mib-1 destas neoplasias, e estabelecer seu valor prognóstico. Neste trabalho foi determinado retrospectivamente o índice de proliferação celular de tumores extraídos de 22 pacientes portadores de meduloblastoma da fossa craniana posterior, tratados no Departamento de Neurocirurgia do Hospital A.C. Camargo de S. Paulo, no período de janeiro de 90 a dezembro de 99. O diagnóstico histopatológico de meduloblastoma foi confirmado pela coloração pela hematoxilina e eosina (HE) e o IP foi determinado através do marcador tumoral anticorpo monoclonal Mib1, que detecta as células em proliferação tumoral nas fases G1, G2, S e M do ciclo celular. Os resultados mostraram que a média do IP Mib1 foi de 30,1%, e variou de 5,2% a 62,0%. A conclusão é que este método tem valor prognóstico, deve ser realizado como rotina no diagnóstico anatomopatológico dos pacientes portadores de meduloblastoma e que aqueles com IP Mib1 maior que a média deverão ser submetidos a tratamentos adjuvantes mais agressivos.

Published

2003

39. Stage IV lung carcinoids: spectrum and evolution of proliferation rate, focusing on variants with elevated proliferation indices

Author

Marc Ladanyi, Wei-Chu Lai, Ai Ni, David S. Klimstra, Isabel Ruth Preeshagul, Anna Maria Litvak, Jason C. Chang, Maria Lauren Santos-Zabala, Charles M. Rudin, M.C. Pietanza, Natasha Rekhtman, Patrice Desmeules, Joseph Montecalvo, Amanda Beras, William D. Travis, and Joshua K. Sabari

Subjects

Adult, Male, carcinoid, 0301 basic medicine, Pathology, medicine.medical_specialty, Lung Neoplasms, Mitotic index, Mitosis, Carcinoid Tumor, Article, lung, Pathology and Forensic Medicine, Diagnosis, Differential, 03 medical and health sciences, 0302 clinical medicine, Predictive Value of Tests, Proliferation rate, Biomarkers, Tumor, Mitotic Index, Humans, Medicine, In patient, small cell carcinoma, large cell neuroendocrine carcinoma, Aged, Cell Proliferation, Neoplasm Staging, Aged, 80 and over, MIB1, Lung, business.industry, Middle Aged, medicine.disease, Primary tumor, 3. Good health, Neuroendocrine Carcinomas, Neuroendocrine Tumors, Ki-67 Antigen, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Predictive value of tests, Disease Progression, Ki-67, Female, Stage iv, business

Abstract

The spectrum and evolution of proliferation rates in stage IV lung carcinoids is poorly defined. In particular, there are limited data on the prevalence and characteristics of tumors exceeding the standard upper proliferative criteria—as defined largely based on early-stage carcinoids—in metastatic setting. Sixty-six patients with stage IV lung carcinoids were identified, and all evaluable samples (n = 132; mean 2 samples per patient) were analyzed for mitotic counts and Ki-67 rate. Clinicopathologic and genomic features associated with elevated proliferation rates (>10 mitoses per 2 mm2 and/or >20% hot-spot Ki-67), and evolution of proliferation rates in serial specimens were analyzed. We found that mitoses and/or Ki-67 exceeded the standard criteria in 35 of 132 (27%) samples, primarily (31/35 cases) at metastatic sites. Although neuroendocrine neoplasms with >10 mitoses per 2 mm2 are currently regarded as de facto neuroendocrine carcinomas, the notion that these cases are part of the spectrum of carcinoids was supported by (1) well-differentiated morphology, (2) conventional proliferation rates in other samples from same patient, (3) genetic characteristics, including the lack of RB1/TP53 alterations in all tested samples (n = 19), and (4) median overall survival of 2.7 years, compared to

Published

2019

40. Interlaboratory variability of MIB1 staining in well-differentiated pancreatic neuroendocrine tumors.

Author

Blank, Annika, Wehweck, Laura, Marinoni, Ilaria, Boos, Laura, Bergmann, Frank, Schmitt, Anja, Perren, Aurel, Boos, Laura Amanda, and Schmitt, Anja Maria

Abstract

Neuroendocrine tumors (NET) are routinely graded and staged to judge prognosis. Proliferation index using MIB1 staining has been introduced to assess grading. There are vivid discussions on cutoff definitions, automated counting, and interobserver variability. However, no data exist regarding interlaboratory reproducibility for low proliferation indices which are of importance to discriminate between G1 and G2 NET. We performed MIB1 staining in three different university hospital-based pathology laboratories on a tissue micro array (TMA) of a well-characterized patient cohort, containing pancreatic NET of 61 patients. To calculate the proliferation index, number of positive tumor nuclei was divided by the total number of tumor nuclei. Labeling index was compared to mitotic counts in whole tissue sections and to clinical outcome. Linear regression analysis, intraclass comparison, and log-rank analysis were performed. Intraclass correlation showed moderate-to-fair agreement. Especially low proliferating tumors were affected by interlaboratory differences. Log-rank analysis was performed for each lab and resulted in three different cutoffs (5.0, 3.0, and 0.5 %). Every calculated cutoff stratified the patient cohort to a significant extent for the underlying stain (p < 0.001, <0.001, and <0.001) but showed no or lesser significance when applied to the other stains. Significant and relevant interlab differences for MIB1 exist. Since the MIB1 proliferation index influences grading, local cutoffs or external standardization should urgently be introduced to achieve reliability and reproducibility. [ABSTRACT FROM AUTHOR]

Published

2015

41. A retrospective study of correlation of morphologic patterns, MIB1 proliferation index, and survival analysis in 134 cases of plasmacytoma.

Author

Ghodke, Kiran, Shet, Tanuja, Epari, Sridhar, Sengar, Manju, Menon, Hari, and Gujral, Sumeet

Abstract

Plasmacytoma classified into solitary plasmacytoma of bone (SPB) and extramedullary plasmacytoma (EMP) is characterized by infiltrate of plasma cells of diverse maturity and by their monoclonal immunoglobulin products. Both SPB and EMP represent different groups of neoplasm in terms of location, tumor progression, and overall survival rate. There is a need for features that indicate likelihood of myeloma in patients with plasmacytoma without other manifestations. This study was an attempt to study the morphologic patterns of plasmacytoma (SPB and EMP), MIB1 proliferation index, and correlation of these with clinicopathologic features and survival of the patients. The study group comprised of 134 cases of plasmacytoma (88 SPB and 46 EMP) over duration of 8 years and were graded as per Bartl's histologic grading system. Commonest site was vertebral body in SPB (36%) and upper aerodigestive tract in EMP (48%). On serum electrophoresis, overall M band was detected in 41% cases. Both SPB and EMP on histology revealed similar morphologic features. MIB1 proliferation index ranged from less than 1% to 80%. It was slightly higher in EMP in comparison with SPB ( P value = .002). Seventy percent of cases, which progressed to multiple myeloma (MM) showed MIB1 labeling index more than 10%; however, it was not statistically significant in predicting the disease progression. With the median follow-up of 19 months (range, 1-99 months), 10 SPB had disease progression of which 7 converted to MM, and 3 developed EMP, with a median interval of 21 months (range, 8-75 months) for the development of MM and 3 months (range, 3-9 months) for the progression to EMP. Five-year survival for EMP varied by site, with poorest survival in brain/central nervous system EMP as compared with EMP at other sites. To conclude, grade and MIB1 proliferation index help in predicting aggressive course in plasmacytoma. [ABSTRACT FROM AUTHOR]

Published

2015

42. Notch signaling is a critical initiator of roof plate formation as revealed by the use of RNA profiling of the dorsal neural tube

Author

Quenten Schwarz, Sophie Wiszniak, Markus Tondl, Sarah Kagan, Chaya Kalcheim, Shai Ofek, Ofek, Shai, Wiszniak, Sophie, Kagan, Sarah, Tondl, Markus, Schwarz, Quenten, and Kalcheim, Chaya

Subjects

Neural Tube, Notch, Quail embryos, Interneuron, QH301-705.5, Physiology, Population, Fate segregation, Notch signaling pathway, Plant Science, General Biochemistry, Genetics and Molecular Biology, Transcriptome, Mice, Neural crest, Structural Biology, biology.animal, medicine, Animals, BMP, Prospective Studies, Biology (General), education, Ecology, Evolution, Behavior and Systematics, education.field_of_study, Mib1, biology, Mouse embryos, Embryogenesis, Neural tube, Gene Expression Regulation, Developmental, Cell Differentiation, Cell Biology, Roof plate formation, fate segregation, Quail, dorsal interneurons, Cell biology, medicine.anatomical_structure, RNA, Dorsal interneurons, delta1, General Agricultural and Biological Sciences, notch, Research Article, Developmental Biology, Biotechnology

Abstract

BackgroundThe dorsal domain of the neural tube is an excellent model to investigate the generation of complexity during embryonic development. It is a highly dynamic and multifaceted region being first transiently populated by prospective neural crest (NC) cells that sequentially emigrate to generate most of the peripheral nervous system. Subsequently, it becomes the definitive roof plate (RP) of the central nervous system. The RP, in turn, constitutes a patterning center for dorsal interneuron development. The factors underlying establishment of the definitive RP and its segregation from NC and dorsal interneurons are currently unknown.ResultsWe performed a transcriptome analysis at trunk levels of quail embryos comparing the dorsal neural tube at premigratory NC and RP stages. This unraveled molecular heterogeneity between NC and RP stages, and within the RP itself. By implementing these genes, we asked whether Notch signaling is involved in RP development. First, we observed that Notch is active at the RP-interneuron interface. Furthermore, gain and loss of Notch function in quail and mouse embryos, respectively, revealed no effect on early NC behavior. Constitutive Notch activation caused a local downregulation of RP markers with a concomitant development of dI1 interneurons, as well as an ectopic upregulation of RP markers in the interneuron domain. Reciprocally, in mice lacking Notch activity, both the RP and dI1 interneurons failed to form and this was associated with expansion of the dI2 population.ConclusionsCollectively, our results offer a new resource for defining specific cell types, and provide evidence that Notch is required to establish the definitive RP, and to determine the choice between RP and interneuron fates, but not the segregation of RP from NC.

Published

2020

43. Immunohistochemical assessment of Ki67 with antibodies SP6 and MIB1 in primary breast cancer: a comparison of prognostic value and reproducibility.

Author

Ekholm, Maria, Beglerbegovic, Sanda, Grabau, Dorthe, Lövgren, Kristina, Malmström, Per, Hartman, Linda, and Fernö, Mårten

Subjects

*CANCER in women, *IMMUNOGLOBULINS, *IMMUNOLOGICAL adjuvants, *TUMORS, *CANCER

Abstract

Aims To compare SP6 and MIB1 antibodies for assessment of Ki67 in primary breast cancer with regard to prognostic value and reproducibility. Methods and results A cohort of 237 premenopausal women with node-negative breast cancer, mainly (87%) not treated with adjuvant systemic therapy, was used. Assessment of Ki67 ( SP6 and MIB1) was performed on tissue microarray by three different investigators. The seventh decile was applied for cut-off. Distant disease-free survival ( DDFS) was chosen as endpoint and the follow-up was restricted to 5 years. Eighty-nine per cent of the samples were classified into the same proliferation group, irrespective of antibody used. For both antibodies, high Ki67 was associated with inferior DDFS in univariable analyses ( SP6: HR 2.5, P = 0.01; and MIB1: HR 2.8, P = 0.004), but failed to reach statistical significance for DDFS in multivariable analyses adjusted for HER2, age, and tumour size ( SP6: HR 2.0, P = 0.074; and MIB1: HR 2.2, P = 0.058). The agreement between different assessors was somewhat higher for MIB1 than for SP6 (κ 0.83-0.88 versus 0.72-0.77). Conclusions SP6 was not superior to MIB1, but the two antibodies were comparable in the assessment of Ki67. Both MIB1 and SP6 could therefore be considered for prognostic use in primary breast cancer. [ABSTRACT FROM AUTHOR]

Published

2014

44. Aberrant DNA methylation of integrin α4 in human breast cancer.

Author

Do, Sung-Im, Ko, Eunkyung, Kang, So, Lee, Jeong, Nam, Seok, Cho, Eun, and Kim, Duk-Hwan

Abstract

Integrins are cell surface receptors that mediate cell-cell/extracellular interactions and have shown an association with metastasis or transformation in several cancers. However, the correlation between the clinicopathological status of breast cancer and the altered integrin α4 status is not clear. In this study, we investigated DNA methylation of integrin α4 in breast cancer. We retrieved 351 cases of surgically resected breast cancer (290 invasive carcinoma and 61 intraductal carcinoma). Methylation-specific polymerase chain reaction was performed to determine integrin α4 methylation status. Integrin α4 methylation was frequently observed in breast cancer specimens (145/351 cases, 41.3 %). In addition, DNA methylation of integrin α4 showed statistical correlation with HER2 positivity and higher histologic grade ( p = 0.001, 0.008 in ductal carcinoma in situ and 0.003 in invasive ductal carcinoma). However, other clinicopathological data such as estrogen receptor, progesterone receptor, metastasis, and TNM status showed no statistical correlation. Moreover, we found that the downregulated expression of integrin α4 in a heavily methylated breast cancer cell line (ZR-75) was restored by treatment with 5-aza-2'deoxycytidine, a DNA methyltransferase inhibitor, implying transcriptional silencing by DNA methylation. We observed that integrin α4 methylation is associated with the histologic grade of tumors and lymph node metastasis. Also, this data supports a previous study that suggested integrin α4 and HER2 are involved in the same signaling pathway. DNA methylation of integrin α4 may be a poor prognostic factor which affects undifferentiated histologic change of breast cancer. [ABSTRACT FROM AUTHOR]

Published

2014

45. Karyopherin a2 and chromosome region maintenance protein 1 expression in meningiomas: novel biomarkers for recurrence and malignant progression.

Author

Gousias, Konstantinos, Niehusmann, Pitt, Gielen, Gerrit, and Simon, Matthias

Abstract

The karyopherin protein family comprises importins and exportins which are nucleocytoplasmic shuttling receptors. Increased levels of karyopherin a2 and chromosome region maintenance protein 1 correlate with a higher WHO grade and a poorer prognosis in patients with infiltrative astrocytomas. The aim of this study was to evaluate representative members of importins and exportins (i.e. karyopherin a2 and chromosome region maintenance protein 1) as novel biomarkers for meningiomas of WHO grades I-III. We semiquantitatively analyzed nuclear expression of karyopherin a2, chromosome region maintenance protein 1 and the MIB1 labeling index using immunohistochemistry in 108 primary (44 meningiomas WHO grade I, 48 meningiomas WHO grade II, 16 meningiomas WHO grade III) and 13 recurrent meningiomas. Statistical analysis was performed using standard techniques. Karyopherin a2 ( p < 0.001) and chromosome region maintenance protein 1 ( p = 0.002) expression correlated significantly with the histological grade. Karyopherin a2 expression correlated with proliferative activity as assessed by the MIB1 index ( p < 0.001). Recurrent tumors expressed significantly higher levels of karyopherin a2 ( p = 0.045) when compared to primary growths. Multivariate analysis of the overall series as well as of patients with atypical meningiomas identified higher karyopherin a2 (≥5 vs. <5 %) and chromosome region maintenance protein 1 (≥60 vs. 60 %) expression as independent predictors of tumor recurrence. Karyopherin a2 and chromosome region maintenance protein 1 expression may have potential as novel biomarkers for meningiomas. [ABSTRACT FROM AUTHOR]

Published

2014

46. Notch signaling represents an important checkpoint between follicular T-helper and canonical T-helper 2 cell fate

Author

R. Lee Reinhardt and Mark Dell'Aringa

Subjects

0301 basic medicine, Notch, T helper 2, Ubiquitin-Protein Ligases, Cellular differentiation, Immunology, Cell, Notch signaling pathway, Tfh, Biology, Cell fate determination, Article, Mice, Th2, 03 medical and health sciences, Th2 Cells, T-Lymphocyte Subsets, Allergic inflammation, medicine, Animals, Immunology and Allergy, Cell Lineage, Receptor, Notch2, T follicular helper cell, Cells, Cultured, Interleukin 4, Strongylida Infections, Mice, Knockout, Mind bomb1, Mib1, Follicular dendritic cells, IL-4, Germinal center, Cell Differentiation, Type-2 immunity, Dendritic Cells, Germinal Center, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Interleukin-4, Nippostrongylus, Signal transduction, Signal Transduction

Abstract

Type-2 immunity is regulated by two distinct CD4+ T cell subsets. T follicular helper (Tfh) cells are required for humoral hallmarks of type-2 inflammation. T helper type-2 (Th2) cells orchestrate type-2 inflammation in peripheral tissues, such as the lung and intestine. Given the importance of Notch signaling in the establishment of other CD4+ T-helper cell subsets, we investigated whether canonical Notch activation could differentially impact Tfh and Th2 cell fate during the induction of type-2 immunity. These studies show that Tfh cell, but not Th2 cell, generation and function is reliant on Notch signaling. While early Tfh cell specification is influenced by functional Notch ligands on classical dendritic cells, functional Notch ligands on cells other than dendritic cells, T cells, B cells, and follicular dendritic cells are sufficient to achieve full Tfh cell commitment. These findings identify Notch signaling as an early lineage-determining factor between Tfh and Th2 cell fate.

Published

2018

47. Cell proliferation markers in the transplanted canine transmissible venereal tumor.

Author

Santos, F. G. A., Moro, L., Cassali, G. D., Paixão, T. A., Campos, P. P., Silva, S. S., and Vasconcelos, A. C.

Subjects

CELL proliferation, LABORATORY dogs, TUMORS, ANTIGENS, CELL nuclei

Abstract

The article discusses a research study on comparing markers of cell proliferation in transplanted canine transmissible venereal tumor (TVT). Twelve tumor specimens were examined through the argyrophilic nucleolar organizing regions (AgNOR) technique or staining with Schorr or immunolabelling for Ki-67 antigen (MIB1). Results showed confinement of MIB1 labeling in the nucleus while the AgNOR index on proliferation had positive correlation to the mitotic index and MIB1 immunolabeling.

Published

2011

48. Usefulness of thallium-201 SPECT in the evaluation of tumor natures in intracranial meningiomas.

Author

Takeda, Tetsuji, Nakano, Takahiro, Asano, Kenichiroh, Shimamura, Norihito, and Ohkuma, Hiroki

Subjects

*MENINGIOMA, *PREOPERATIVE care, *RADIOISOTOPES, *STATISTICS, *THALLIUM isotopes, *U-statistics, *DECISION making in clinical medicine, *DATA analysis, *SINGLE-photon emission computed tomography, *RECEIVER operating characteristic curves, *ENDOTHELIAL growth factors, *DATA analysis software, *PROGNOSIS, CENTRAL nervous system tumors

Abstract

Introduction: Although intracranial meningiomas are regarded as benign tumors, some of them behave clinically as malignant tumors. Past reports suggest that MIB 1 and vascular endothelial growth factor (VEGF) in postoperative tumor specimens correlate with the aggressive nature of tumors, but preoperative prediction of such a nature is more useful for therapeutic planning for the tumor. The purpose of this study was to assess the usefulness of preoperative thallium-201 chloride single-photon emission computed tomography (Tl SPECT) to evaluate biological behavior in intracranial meningiomas. Methods: Tl SPECT was performed on 39 patients with intracranial meningioma and Tl uptake indices were calculated. The difference in the Tl uptake index between atypical meningiomas and other pathological types of meningioma was evaluated. Moreover, correlation of Tl uptake indices with the MIB1 labeling index was estimated. Tl uptake indices were also compared between VEGF strongly positive and weakly positive meningiomas. Results: The delayed index of atypical meningioma was significantly higher than that of the other pathological types ( p = 0.036). Significant correlation was found between the Tl uptake index in the delayed image and MIB1 labeling index ( p < 0.0001, R = 0.36). Moreover, VEGF strongly positive meningiomas exhibited a significantly higher Tl uptake index compared to VEGF weakly positive meningiomas in both the early image and the delayed image ( p = 0.029, 0.023, respectively). Conclusions: Tl uptake index may be a possible preoperative surrogate marker of MIB1 and VEGF that is useful in detecting aggressive natures in intracranial meningiomas. [ABSTRACT FROM AUTHOR]

Published

2011

49. Endoscopic appearance of GERD: Putative role of cell proliferation.

Author

Calabrese, C., Trerè, D., Fabbri, A., Cenacchi, G., Vici, M., Derenzini, M., and Di Febo, G.

Subjects

ENDOSCOPY, GASTROESOPHAGEAL reflux, ESOPHAGUS diseases, CELL proliferation

Abstract

Abstract: Background: Erosive esophagitis is a frequent endoscopic feature in patients with gastro-oesophageal reflux disease. However, most of patients with heartburn/regurgitation have a non-erosive reflux disease. The reason for this heterogeneous impact of gastro-oesophageal reflux disease on oesophageal mucosa is unknown to date. Aim: To evaluate the cell proliferation status of oesophageal epithelium in both healthy normal subjects and patients with gastro-oesophageal reflux disease with or without erosions. Materials and methods: All the subjects underwent endoscopy and biopsies were taken at 5cm from the squamo-columnar junction. Specimens were analysed both at histology and at transmission electron microscopy. Cell proliferation was evaluated by MIB1 immunostaining. Of the 85 subjects were studied, 10 were healthy controls with normal pH-testing and macroscopical, histological and ultrastructural patterns; 37were patients with erosive esophagitis, and 38 patients with non-erosive reflux disease. Results: At histology, of the 37 patients affected by erosive esophagitis, 30 had normal mucosa and 7 showed mild oesophagitis. One patient with non-erosive reflux disease showed signs of oesophagitis at histology. At TEM, all patients with gastro-oesophageal reflux disease had ultrastructural patterns of damage i.e. dilations of intercellular spaces (DIS), and all controls had a normal ultrastructural pattern. The mean (±SD) MIB1-LI values of normal subjects and non-erosive reflux disease and erosive oesophagitis patients were 62.2% (±9.1), 29.7% (±7.2) and 16.2% (±5.2), respectively; there were significant differences among the three groups (p <0.001). Conclusions: Oesophageal mucosa of patients with reflux symptoms presents a decrease in MIB1 immunostaining of 50% and 25% in non-erosive reflux disease and erosive esophagitis patients with respect to normal subjects. [Copyright &y& Elsevier]

Published

2007

50. The impact of c-kit mutations on histomorphological risk assessment of gastrointestinal stromal tumors.

Author

Koelz, M., Wick, N., Winkler, T., Längle, F., and Wrba, F.

Abstract

Copyright of European Surgery: ACA Acta Chirurgica Austriaca is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2007