Your search keyword '"Tangliang Li"' showing total 36 results

1. Fine-tuning of Wnt signaling by RNA surveillance factor Smg5 in the mouse craniofacial development

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Author

Shicheng Zhu, Suman Huo, Weiran He, Caiyan Huang, Jiannan Zhang, Xiaoning Jiang, Yeqing Qian, Chengyan Chen, Zhong-Min Dai, Xueqin Yang, Mengsheng Qiu, Tangliang Li, and Xiao-Jing Zhu

Subjects

Pathophysiology, Cell biology, Developmental biology, Science

Abstract

Summary: The specific roles of nonsense-mediated mRNA decay (NMD), a translation-dependent RNA quality control mechanism that degrades mRNAs containing premature termination codons (PTCs), in mammalian craniofacial development have remained unclear. Here, we show that knockout of the essential NMD factor Smg5 in mouse craniofacial neural crest cells leads to hypoplastic mandibles, subsequently inducing tongue mispositioning and cleft palate formation. Furthermore, Smg5 loss triggers massive cell apoptosis and disrupts cell differentiation, accompanied by widespread alterations in alternative splicing and a surge in PTC-containing mRNA levels. Notably, the abnormal upregulation of a PTC-containing Porcn transcript leads to reduced Porcn protein and impaired Wnt5a/JNK signaling, a crucial pathway for craniofacial morphogenesis. Finally, death of Smg5-deficient craniofacial neural crest cells can be ameliorated by Wnt5a in craniofacial neural crest (CNC) in vitro explants. Taken together, our findings demonstrate that Smg5-mediated NMD regulates mammalian craniofacial development by fine-tuning Wnt signaling through post-transcriptional regulation of Porcn. more...

Published

2025

2. RNA Surveillance Factor SMG5 Is Essential for Mouse Embryonic Stem Cell Differentiation

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Author

Chengyan Chen, Yanling Wei, Xiaoning Jiang, and Tangliang Li

Subjects

nonsense-mediated mRNA decay, mouse embryonic stem cells, SMG5, c-MYC, differentiation, Microbiology, QR1-502

Abstract

Nonsense-mediated mRNA decay (NMD) is a highly conserved post-transcriptional gene expression regulatory mechanism in eukaryotic cells. NMD eliminates aberrant mRNAs with premature termination codons to surveil transcriptome integrity. Furthermore, NMD fine-tunes gene expression by destabilizing RNAs with specific NMD features. Thus, by controlling the quality and quantity of the transcriptome, NMD plays a vital role in mammalian development, stress response, and tumorigenesis. Deficiencies of NMD factors result in early embryonic lethality, while the underlying mechanisms are poorly understood. SMG5 is a key NMD factor. In this study, we generated an Smg5 conditional knockout mouse model and found that Smg5-null results in early embryonic lethality before E13.5. Furthermore, we produced multiple lines of Smg5 knockout mouse embryonic stem cells (mESCs) and found that the deletion of Smg5 in mESCs does not compromise cell viability. Smg5-null delays differentiation of mESCs. Mechanistically, our study reveals that the c-MYC protein, but not c-Myc mRNA, is upregulated in SMG5-deficient mESCs. The overproduction of c-MYC protein could be caused by enhanced protein synthesis upon SMG5 loss. Furthermore, SMG5-null results in dysregulation of alternative splicing on multiple stem cell differentiation regulators. Overall, our findings underscore the importance of SMG5-NMD in regulating mESC cell-state transition. more...

Published

2024

3. Editorial: RNA metabolism and DNA stability in the central nervous system (CNS): from aging to neurodegenerative disease

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Author

Tangliang Li, Wenting Guo, and Haibo Wang

Subjects

RNA metabolism, DNA stability, PARP1, miRNA, Alzheimer’s disease, Biology (General), QH301-705.5

Published

2024

4. Poly(ADP-Ribose) Polymerase-1 Lacking Enzymatic Activity Is Not Compatible with Mouse Development

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Author

Tatiana Kamaletdinova, Wen Zong, Pavel Urbánek, Sijia Wang, Mara Sannai, Paulius Grigaravičius, Wenli Sun, Zahra Fanaei-Kahrani, Aswin Mangerich, Michael O. Hottiger, Tangliang Li, and Zhao-Qi Wang

Subjects

PARP1, PARP2, catalytic activity, development, ES cell differentiation, genotoxic stress, Cytology, QH573-671

Abstract

Poly(ADP-ribose) polymerase-1 (PARP1) binds DNA lesions to catalyse poly(ADP-ribosyl)ation (PARylation) using NAD+ as a substrate. PARP1 plays multiple roles in cellular activities, including DNA repair, transcription, cell death, and chromatin remodelling. However, whether these functions are governed by the enzymatic activity or scaffolding function of PARP1 remains elusive. In this study, we inactivated in mice the enzymatic activity of PARP1 by truncating its C-terminus that is essential for ART catalysis (PARP1ΔC/ΔC, designated as PARP1-ΔC). The mutation caused embryonic lethality between embryonic day E8.5 and E13.5, in stark contrast to PARP1 complete knockout (PARP1−/−) mice, which are viable. Embryonic stem (ES) cell lines can be derived from PARP1ΔC/ΔC blastocysts, and these mutant ES cells can differentiate into all three germ layers, yet, with a high degree of cystic structures, indicating defects in epithelial cells. Intriguingly, PARP1-ΔC protein is expressed at very low levels compared to its full-length counterpart, suggesting a selective advantage for cell survival. Noticeably, PARP2 is particularly elevated and permanently present at the chromatin in PARP1-ΔC cells, indicating an engagement of PARP2 by non-enzymatic PARP1 protein at the chromatin. Surprisingly, the introduction of PARP1-ΔC mutation in adult mice did not impair their viability; yet, these mutant mice are hypersensitive to alkylating agents, similar to PARP1−/− mutant mice. Our study demonstrates that the catalytically inactive mutant of PARP1 causes the developmental block, plausibly involving PARP2 trapping. more...

Published

2023

5. Lessons from the diet: Captivity and sex shape the gut microbiota in an oviparous lizard (Calotes versicolor)

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Author

Lin Zhang, Fang Yang, Tangliang Li, Buddhi Dayananda, Longhui Lin, and Chixian Lin

Subjects

Calotes versicolor, captivity, diet, gut microbiota, sex, Ecology, QH540-549.5

Abstract

Abstract Studies have indicated that the abundance and community structure of gut microbiota are altered by diet. In this study, next‐generation sequencing of the 16S rRNA gene amplicon was performed to evaluate variations in the gut microbiota of wild and captive individuals of both sexes of Calotes versicolor. The results showed that there was a significant sex difference in microbial community structure for wild C. versicolor, Bacteroide was the dominant genus in wild females (WF), whereas Ochrobactrum was the dominant genus in wild males (WM). Acinetobacter and Hymenobacter were the dominant genera in WF, while Clostridium was the dominant genus in captive females (CF). The results indicated that differences in diet between wild and captive C. versicolor also resulted in variations in gut microbiota. Thus, it was not surprising that captivity and sex shape the gut microbiota in C. versicolor. In summary, the fundamental information presented about the gut microbiota of both sexes of wild (and captive females) C. versicolor, indicates that the artificial environments are not suitable for the wild C. versicolor. more...

Published

2022

6. The Central Domain of MCPH1 Controls Development of the Cerebral Cortex and Gonads in Mice

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Author

Yaru Wang, Wen Zong, Wenli Sun, Chengyan Chen, Zhao-Qi Wang, and Tangliang Li

Subjects

microcephaly, MCPH1, central domain, brain development, gonad development, Cytology, QH573-671

Abstract

MCPH1 is the first gene identified to be responsible for the human autosomal recessive disorder primary microcephaly (MCPH). Mutations in the N-terminal and central domains of MCPH1 are strongly associated with microcephaly in human patients. A recent study showed that the central domain of MCPH1, which is mainly encoded by exon 8, interacts with E3 ligase βTrCP2 and regulates the G2/M transition of the cell cycle. In order to investigate the biological functions of MCPH1’s central domain, we constructed a mouse model that lacked the central domain of MCPH1 by deleting its exon 8 (designated as Mcph1-Δe8). Mcph1-Δe8 mice exhibited a reduced brain size and thinner cortex, likely caused by a compromised self-renewal capacity and premature differentiation of Mcph1-Δe8 neuroprogenitors during corticogenesis. Furthermore, Mcph1-Δe8 mice were sterile because of a loss of germ cells in the testis and ovary. The embryonic fibroblasts of Mcph1-Δe8 mice exhibited premature chromosome condensation (PCC). All of these findings indicate that Mcph1-Δe8 mice are reminiscent of MCPH1 complete knockout mice and Mcph1-ΔBR1 mice. Our study demonstrates that the central domain of MCPH1 represses microcephaly, and is essential for gonad development in mammals. more...

Published

2022

7. DNA Damage Response in Hematopoietic Stem Cell Ageing

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Author

Tangliang Li, Zhong-Wei Zhou, Zhenyu Ju, and Zhao-Qi Wang

Subjects

Hematopoietic stem cells, DNA damage response, Epigenetics, Ageing, P53, Biology (General), QH301-705.5, Computer applications to medicine. Medical informatics, R858-859.7

Abstract

Maintenance of tissue-specific stem cells is vital for organ homeostasis and organismal longevity. Hematopoietic stem cells (HSCs) are the most primitive cell type in the hematopoietic system. They divide asymmetrically and give rise to daughter cells with HSC identity (self-renewal) and progenitor progenies (differentiation), which further proliferate and differentiate into full hematopoietic lineages. Mammalian ageing process is accompanied with abnormalities in the HSC self-renewal and differentiation. Transcriptional changes and epigenetic modulations have been implicated as the key regulators in HSC ageing process. The DNA damage response (DDR) in the cells involves an orchestrated signaling pathway, consisting of cell cycle regulation, cell death and senescence, transcriptional regulation, as well as chromatin remodeling. Recent studies employing DNA repair-deficient mouse models indicate that DDR could intrinsically and extrinsically regulate HSC maintenance and play important roles in tissue homeostasis of the hematopoietic system. In this review, we summarize the current understanding of how the DDR determines the HSC fates and finally contributes to organismal ageing. more...

Published

2016

8. A First Generation Comparative Chromosome Map between Guinea Pig (Cavia porcellus) and Humans.

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Author

Svetlana A Romanenko, Polina L Perelman, Vladimir A Trifonov, Natalia A Serdyukova, Tangliang Li, Beiyuan Fu, Patricia C M O'Brien, Bee L Ng, Wenhui Nie, Thomas Liehr, Roscoe Stanyon, Alexander S Graphodatsky, and Fengtang Yang more...

Subjects

Medicine, Science

Abstract

The domesticated guinea pig, Cavia porcellus (Hystricomorpha, Rodentia), is an important laboratory species and a model for a number of human diseases. Nevertheless, genomic tools for this species are lacking; even its karyotype is poorly characterized. The guinea pig belongs to Hystricomorpha, a widespread and important group of rodents; so far the chromosomes of guinea pigs have not been compared with that of other hystricomorph species or with any other mammals. We generated full sets of chromosome-specific painting probes for the guinea pig by flow sorting and microdissection, and for the first time, mapped the chromosomal homologies between guinea pig and human by reciprocal chromosome painting. Our data demonstrate that the guinea pig karyotype has undergone extensive rearrangements: 78 synteny-conserved human autosomal segments were delimited in the guinea pig genome. The high rate of genome evolution in the guinea pig may explain why the HSA7/16 and HSA16/19 associations presumed ancestral for eutherians and the three syntenic associations (HSA1/10, 3/19, and 9/11) considered ancestral for rodents were not found in C. porcellus. The comparative chromosome map presented here is a starting point for further development of physical and genetic maps of the guinea pig as well as an aid for genome assembly assignment to specific chromosomes. Furthermore, the comparative mapping will allow a transfer of gene map data from other species. The probes developed here provide a genomic toolkit, which will make the guinea pig a key species to unravel the evolutionary biology of the Hystricomorph rodents. more...

Published

2015

9. UPF3A is a ubiquitously expressed NMD factor among mouse tissues

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Author

Xin Ma, Yan Li, Chengyan Chen, and Tangliang Li

Abstract

Nonsense-mediated mRNA decay (NMD), an important post-transcriptional regulatory mechanism in gene expression, is actively involved in a series of cellular and physiological processes, thus controlling cell fate and tissue homeostasis. Defects in NMD cause human diseases such as neurodevelopmental disorders, tumorigenesis and autoimmunity. UPF3 (Up- frameshift protein 3), first identified in the baker’s yeast, is a core NMD factor. UPF3A and UPF3B, the two UPF3 paralogs emerging in vertebrates, have either activating or suppressing roles in NMD. Previous studies found that UPF3B protein is ubiquitously expressed in almost all mammalian organs, while UPF3A protein is hardly detectable in most of mammalian tissues, except in the testis. One hypothesis explaining this phenomena is the functional antognism between UPF3A and UPF3B in NMD. Thus, UPF3B competitively binds to UPF2 with higher affinity than UPF3A, which finally destabilizes UPF3A protein. In the present study, we quantitatively evaluated the expression of UPF3A and UPF3B in nine major tissues and reproductive organs of wild type male and female mice. Our study confirmed that UPF3A has the highest expression in male germlines. To our surprise, we found in most tissues, including brain and thymus, the protein level of UPF3A is comparable with that of UPF3B. In spleen and lung, UPF3A is higher than UPF3B. These findings are further supported by publicly available gene expression data. Thus, our study demonstrated that UPF3A protein is ubiquitously expressed in mouse tissues, and may play important roles in the homeostasis of multiple mammalian tissues. more...

Published

2023

10. UPF3A is dispensable for nonsense-mediated mRNA decay in mouse pluripotent and somatic cells

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Author

Chengyan Chen, Yanmin Shen, Luqian Li, Yaoxin Ren, Zhao-Qi Wang, and Tangliang Li

Subjects

Ecology, Health, Toxicology and Mutagenesis, Plant Science, Biochemistry, Genetics and Molecular Biology (miscellaneous)

Abstract

Nonsense-mediated mRNA decay (NMD) is a highly conserved regulatory mechanism of post-transcriptional gene expression in eukaryotic cells. NMD plays essential roles in mRNA quality and quantity control, and thus safeguards multiple biological processes including embryonic stem cell differentiation and organogenesis. UPF3A and UPF3B in vertebrate species, originated from a singleUPF3gene in yeast, are key factors in the NMD machinery. While UPF3B is a well-recognized weak NMD-promoting factor, whether UPF3A functions in promoting or suppressing NMD is under debate. In this study, we generated aUpf3aconditional knockout mouse strain, and established multiple lines of embryonic stem cells and somatic cells without UPF3A. Through extensive analysis on the expressions of 33 NMD targets, we found UPF3A neither represses NMD in mouse embryonic stem cells, somatic cells, nor in major organs including the liver, spleen, and thymus. Our study reinforces that UPF3A is dispensable for NMD when UPF3B is present. Furthermore, UPF3A may weakly and selectively promote NMD in certain murine organs.Summary blurbWe generated a newUpf3ainducible knockout mouse model and showed that UPF3A does not repress expressions of NMD target genes in embryonic stem cells, somatic fibroblasts, as well as multiple tissues from adult mice. more...

Published

2022

11. NBS1 interacts with Notch signaling in neuronal homeostasis

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Author

Tina Rüdiger, George Yakoub, Christoph Kaether, Tangliang Li, Kanstantsin Siniuk, Ruiqing Lu, Murat Kirtay, Nadine Schneble, Zhong-Wei Zhou, Yi-Nan Jiang, Mingmei Ding, Ari Barzilai, and Zhao-Qi Wang

Subjects

Genome instability, DNA Repair, AcademicSubjects/SCI00010, Neurogenesis, Notch signaling pathway, Cell Cycle Proteins, Genome Integrity, Repair and Replication, Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Animals, Cells, Cultured, 030304 developmental biology, Neurons, MRE11 Homologue Protein, 0303 health sciences, Receptors, Notch, Effector, Fibroblasts, Embryo, Mammalian, medicine.disease, Acid Anhydride Hydrolases, Cell biology, DNA-Binding Proteins, Crosstalk (biology), Rad50, Signal transduction, 030217 neurology & neurosurgery, Nijmegen breakage syndrome, DNA Damage

Abstract

NBS1 is a critical component of the MRN (MRE11/RAD50/NBS1) complex, which regulates ATM- and ATR-mediated DNA damage response (DDR) pathways. Mutations in NBS1 cause the human genomic instability syndrome Nijmegen Breakage Syndrome (NBS), of which neuronal deficits, including microcephaly and intellectual disability, are classical hallmarks. Given its function in the DDR to ensure proper proliferation and prevent death of replicating cells, NBS1 is essential for life. Here we show that, unexpectedly, Nbs1 deletion is dispensable for postmitotic neurons, but compromises their arborization and migration due to dysregulated Notch signaling. We find that Nbs1 interacts with NICD-RBPJ, the effector of Notch signaling, and inhibits Notch activity. Genetic ablation or pharmaceutical inhibition of Notch signaling rescues the maturation and migration defects of Nbs1-deficient neurons in vitro and in vivo. Upregulation of Notch by Nbs1 deletion is independent of the key DDR downstream effector p53 and inactivation of each MRN component produces a different pattern of Notch activity and distinct neuronal defects. These data indicate that neuronal defects and aberrant Notch activity in Nbs1-deficient cells are unlikely to be a direct consequence of loss of MRN-mediated DDR function. This study discloses a novel function of NBS1 in crosstalk with the Notch pathway in neuron development. more...

Published

2020

12. PARP1: Liaison of Chromatin Remodeling and Transcription

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Author

Wen, Zong, Yamin, Gong, Wenli, Sun, Tangliang, Li, and Zhao-Qi, Wang

Abstract

Poly(ADP-ribosyl)ation (PARylation) is a covalent post-translational modification and plays a key role in the immediate response of cells to stress signals. Poly(ADP-ribose) polymerase 1 (PARP1), the founding member of the PARP superfamily, synthesizes long and branched polymers of ADP-ribose (PAR) onto acceptor proteins, thereby modulating their function and their local surrounding. PARP1 is the most prominent of the PARPs and is responsible for the production of about 90% of PAR in the cell. Therefore, PARP1 and PARylation play a pleotropic role in a wide range of cellular processes, such as DNA repair and genomic stability, cell death, chromatin remodeling, inflammatory response and gene transcription. PARP1 has DNA-binding and catalytic activities that are important for DNA repair, yet also modulate chromatin conformation and gene transcription, which can be independent of DNA damage response. PARP1 and PARylation homeostasis have also been implicated in multiple diseases, including inflammation, stroke, diabetes and cancer. Studies of the molecular action and biological function of PARP1 and PARylation provide a basis for the development of pharmaceutic strategies for clinical applications. This review focuses primarily on the role of PARP1 in the regulation of chromatin remodeling and transcriptional activation. more...

Published

2022

13. UPF3A is dispensable for nonsense-mediated mRNA decay in mouse pluripotent and somatic cells.

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Author

Chengyan Chen, Yanmin Shen, Luqian Li, Yaoxin Ren, Zhao-Qi Wang, and Tangliang Li

Published

2023

14. Lessons from the diet: Captivity and sex shape the gut microbiota in an oviparous lizard (

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Author

Lin, Zhang, Fang, Yang, Tangliang, Li, Buddhi, Dayananda, Longhui, Lin, and Chixian, Lin

Abstract

Studies have indicated that the abundance and community structure of gut microbiota are altered by diet. In this study, next-generation sequencing of the 16S rRNA gene amplicon was performed to evaluate variations in the gut microbiota of wild and captive individuals of both sexes of more...

Published

2021

15. Fine-Tuning of PGC1α Expression Regulates Cardiac Function and Longevity

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Author

Joseph Loscalzo, Hu Wang, Zeping Hu, Daojun Diao, Xudong Zhu, Yuzheng Zhao, Bo Liu, Tangliang Li, Lijuan Song, Weiyan Shen, Johan Auwerx, Chengtao Li, Hongbo Zhang, Genxiang Mao, Zhenyu Ju, Yugang Qiu, Yejun Zou, Wengong Wang, Ke Yao, Ping Huang, Yi Yang, and Yong Zhou more...

Subjects

Male, 0301 basic medicine, Telomerase, Bioenergetics, Physiology, media_common.quotation_subject, Longevity, Biology, Mitochondrion, Mitochondria, Heart, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Coactivator, Animals, Homeostasis, Myocytes, Cardiac, Receptor, Cells, Cultured, media_common, Organelle Biogenesis, Autophagy, Peroxisome, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, 030220 oncology & carcinogenesis, Female, Reactive Oxygen Species, Cardiology and Cardiovascular Medicine

Abstract

Rationale: PGC1α (peroxisome proliferator-activated receptor gamma coactivator 1α) represents an attractive target interfering bioenergetics and mitochondrial homeostasis, yet multiple attempts have failed to upregulate PGC1α expression as a therapy, for instance, causing cardiomyopathy. Objective: To determine whether a fine-tuning of PGC1α expression is essential for cardiac homeostasis in a context-dependent manner. Methods and Results: Moderate cardiac-specific PGC1α overexpression through a ROSA26 locus knock-in strategy was utilized in WT (wild type) mice and in G3Terc −/− (third generation of telomerase deficient; hereafter as G3) mouse model, respectively. Ultrastructure, mitochondrial stress, echocardiographic, and a variety of biological approaches were applied to assess mitochondrial physiology and cardiac function. While WT mice showed a relatively consistent PGC1α expression from 3 to 12 months old, age-matched G3 mice exhibited declined PGC1α expression and compromised mitochondrial function. Cardiac-specific overexpression of PGC1α (PGC1α OE ) promoted mitochondrial and cardiac function in 3-month-old WT mice but accelerated cardiac aging and significantly shortened life span in 12-month-old WT mice because of increased mitochondrial damage and reactive oxygen species insult. In contrast, cardiac-specific PGC1α knock in in G3 (G3 PGC1α OE ) mice restored mitochondrial homeostasis and attenuated senescence-associated secretory phenotypes, thereby preserving cardiac performance with age and extending health span. Mechanistically, age-dependent defect in mitophagy is associated with accumulation of damaged mitochondria that leads to cardiac impairment and premature death in 12-month-old WT PGC1α OE mice. In the context of telomere dysfunction, PGC1α induction replenished energy supply through restoring the compromised mitochondrial biogenesis and thus is beneficial to old G3 heart. Conclusions: Fine-tuning the expression of PGC1α is crucial for the cardiac homeostasis because the balance between mitochondrial biogenesis and clearance is vital for regulating mitochondrial function and homeostasis. These results reinforce the importance of carefully evaluating the PGC1α-boosting strategies in a context-dependent manner to facilitate clinical translation of novel cardioprotective therapies. more...

Published

2019

16. Nbs1‐mediated DNA damage repair pathway regulates haematopoietic stem cell development and embryonic haematopoiesis

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Author

Zhao-Qi Wang, Zhenyu Ju, Tangliang Li, Jie Sun, and Yu Chen

Subjects

0301 basic medicine, p53, Programmed cell death, DNA Repair, DNA repair, DNA damage, Cell Cycle Proteins, Cell fate determination, Biology, DNA damage response, Nbs1, 03 medical and health sciences, Mice, 0302 clinical medicine, Animals, Progenitor cell, Haematopoietic stem cells, hemic and immune systems, Cell Differentiation, Cell Biology, General Medicine, Original Articles, Hematopoietic Stem Cells, Embryonic stem cell, Cell biology, Hematopoiesis, DNA-Binding Proteins, Haematopoiesis, 030104 developmental biology, Cell fate, 030220 oncology & carcinogenesis, Original Article, Stem cell, DNA Damage, Signal Transduction

Abstract

Objectives DNA damages pose threats to haematopoietic stem cells (HSC) maintenance and haematopoietic system homeostasis. Quiescent HSCs in adult mouse bone marrow are resistant to DNA damage, while human umbilical cord blood‐derived proliferative HSCs are prone to cell death upon ionizing radiation. Murine embryonic HSCs proliferate in foetal livers and divide symmetrically to generate HSC pool. How murine embryonic HSCs respond to DNA damages is not well‐defined. Materials and methods Mice models with DNA repair molecule Nbs1 or Nbs1/p53 specifically deleted in embryonic HSCs were generated. FACS analysis, in vitro and in vivo HSC differentiation assays, qPCR, immunofluorescence and Western blotting were used to delineate roles of Nbs1‐p53 signaling in HSCs and haematopoietic progenitors. Results Nbs1 deficiency results in persistent DNA breaks in embryonic HSCs, compromises embryonic HSC development and finally results in mouse perinatal lethality. The persistent DNA breaks in Nbs1 deficient embryonic HSCs render cell cycle arrest, while driving a higher rate of cell death in haematopoietic progenitors. Although Nbs1 deficiency promotes Atm‐Chk2‐p53 axis activation in HSCs and their progenies, ablation of p53 in Nbs1 deficient HSCs accelerates embryonic lethality. Conclusions Our study discloses that DNA double‐strand repair molecule Nbs1 is essential in embryonic HSC development and haematopoiesis. Persistent DNA damages result in distinct cell fate in HSCs and haematopoietic progenitors. Nbs1 null HSCs tend to be maintained through cell cycle arrest, while Nbs1 null haematopoietic progenitors commit cell death. The discrepancies are mediated possibly by different magnitude of p53 signaling., Genetic deletion of Nbs1, a DNA double‐strand break repair molecule, in murine embryonic haematopoietic stem cells (HSCs) generates persistent DNA damages in HSCs and their progenies, contributing to defective haematopoiesis and perinatal lethality in mice. Nbs1 null HSCs and haematopoietic progenitors show different cell fate, which could be mediated by differential magnitude of p53 signaling in each cell population. Intriguingly, p53 loss accelerates lethality of mice with Nbs1 deletion in HSCs, indicating an essential role of p53 signaling safeguarding embryonic haematopoiesis. more...

Published

2021

17. Nonsense-mediated mRNA decay: a ‘nonsense’ pathway makes sense in stem cell biology

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Author

Xin Han, Yanling Wei, Feilong Wang, Zhenyu Ju, Hua Wang, and Tangliang Li

Subjects

0301 basic medicine, Somatic cell, Cellular differentiation, Human Embryonic Stem Cells, Nonsense-mediated decay, Biology, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, Neural Stem Cells, Genetics, Humans, Epigenetics, Survey and Summary, Gene, Tissue homeostasis, Cell Proliferation, Cell Differentiation, Hematopoietic Stem Cells, Stem Cell Research, Embryonic stem cell, Nonsense Mediated mRNA Decay, Cell biology, Isoenzymes, Adult Stem Cells, 030104 developmental biology, Codon, Nonsense, Trans-Activators, Stem cell, RNA Helicases

Abstract

Nonsense-mediated mRNA decay (NMD) is a highly conserved post-transcriptional regulatory mechanism of gene expression in eukaryotes. Originally, NMD was identified as an RNA surveillance machinery in degrading ‘aberrant’ mRNA species with premature termination codons. Recent studies indicate that NMD regulates the stability of natural gene transcripts that play significant roles in cell functions. Although components and action modes of the NMD machinery in degrading its RNA targets have been extensively studied with biochemical and structural approaches, the biological roles of NMD remain to be defined. Stem cells are rare cell populations, which play essential roles in tissue homeostasis and hold great promises in regenerative medicine. Stem cells self-renew to maintain the cellular identity and differentiate into somatic lineages with specialized functions to sustain tissue integrity. Transcriptional regulations and epigenetic modulations have been extensively implicated in stem cell biology. However, post-transcriptional regulatory mechanisms, such as NMD, in stem cell regulation are largely unknown. In this paper, we summarize the recent findings on biological roles of NMD factors in embryonic and tissue-specific stem cells. Furthermore, we discuss the possible mechanisms of NMD in regulating stem cell fates. more...

Published

2017

18. The E3 ubiquitin ligase <scp>APC</scp> / <scp> C C </scp> dh1 degrades <scp>MCPH</scp> 1 after MCPH1‐βTr <scp>CP</scp> 2‐Cdc25A‐mediated mitotic entry to ensure neurogenesis

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Author

Xiaoqian Liu, Yujun Wang, Xingzhi Xu, Zhao-Qi Wang, Wen Zong, Tangliang Li, and Zhong-Wei Zhou

Subjects

0301 basic medicine, Mitotic index, Cell cycle checkpoint, General Immunology and Microbiology, Cell division, General Neuroscience, Neurogenesis, Biology, General Biochemistry, Genetics and Molecular Biology, Neural stem cell, Cell biology, Ubiquitin ligase, 03 medical and health sciences, 030104 developmental biology, biology.protein, Ectopic expression, Molecular Biology, Mitosis

Abstract

Mutations of microcephalin (MCPH1) can cause the neurodevelopmental disorder primary microcephaly type 1. We previously showed that MCPH1 deletion in neural stem cells results in early mitotic entry that distracts cell division mode, leading to exhaustion of the progenitor pool. Here, we show that MCPH1 interacts with and promotes the E3 ligase βTrCP2 to degrade Cdc25A independent of DNA damage. Overexpression of βTrCP2 or the knockdown of Cdc25A remedies the high mitotic index and rescues the premature differentiation of Mcph1 ‐deficient neuroprogenitors in vivo . MCPH1 itself is degraded by APC/C C dh1 , but not APC/C C dc20 , in late mitosis and G1 phase. Forced MCPH1 expression causes cell death, underlining the importance of MCPH1 turnover after mitosis. Ectopic expression of Cdh1 leads to premature differentiation of neuroprogenitors, mimicking differentiation defects of Mcph1 ‐knockout neuroprogenitors. The homeostasis of MCPH1 in association with the ubiquitin‐proteasome system ensures mitotic entry independent of cell cycle checkpoint. This study provides a mechanistic understanding of how MCPH1 controls neural stem cell fate and brain development. more...

Published

2017

19. PGC1α protects against hepatic steatosis and insulin resistance via enhancing IL10-mediated anti-inflammatory response

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Author

Ye Feng, Li Chen, Daojun Diao, Weiyan Shen, Zhenyu Ju, Lingling Zhang, Tangliang Li, Xudong Zhu, Chaohui Yu, Peihao Liu, Leiming Liu, Hu Wang, Fan Yang, Weihua Zhou, Xingyong Wan, Jian Ren, Qi Zhao, Jing Li, and Sheng Yan more...

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Anti-Inflammatory Agents, Alpha (ethology), Gene Expression, Inflammation, Protective Agents, Biochemistry, 03 medical and health sciences, Mice, 0302 clinical medicine, Insulin resistance, Internal medicine, Genetics, Medicine, Animals, Neutralizing antibody, Molecular Biology, biology, business.industry, Fatty liver, Lipid metabolism, medicine.disease, Lipid Metabolism, Antibodies, Neutralizing, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Interleukin-10, Mitochondria, Fatty Liver, Interleukin 10, 030104 developmental biology, Endocrinology, Liver, biology.protein, Hepatocytes, Steatosis, medicine.symptom, Insulin Resistance, business, 030217 neurology & neurosurgery, Biotechnology

Abstract

Inflammatory responses are pivotal incidences in hepatic metabolic derangements. However, the underlying mechanism remains elusive. The present study aimed to evaluate the role of peroxisome proliferator-activated receptor-gamma, coactivator 1 alpha (PGC1α) in IL10-mediated anti-inflammatory response, and its role in hepatic steatosis and insulin resistance. Hepatocyte-specific PGC1α knock-in (LivPGC1α) mice and the control mice were fed high-fat diet (HFD) for 8 weeks. IL-10 neutralizing antibody was injected into the liver of PGC1α mice. A variety of biological and histological approaches were applied to assess hepatic function. We demonstrated that hepatic PGC1α expression was significantly reduced in mice fed HFD. LivPGC1α livers exhibited enhanced gene expressions involving mitochondrial function, and favored an accelerated lipid metabolism upon HFD. Meanwhile, LivPGC1α mice revealed improved hepatic steatosis and insulin resistance. Mechanistically, PGC1α bound and activated the promotor region of IL-10, thereby attenuating inflammatory response in the liver. Administration of IL10 neutralizing antibody to LivPGC1α mice abolished PGC1α-mediated anti-inflammatory effects in mice. Further, IL-10 neutralizing antibody intervention aggravated hepatic steatosis and insulin resistance in LivPGC1α mice. Taken together, our data indicated that hepatic-specific overexpression of PGC1α exerts a beneficial role in the regulation of hepatic steatosis and insulin resistance via enhancing IL10-mediated anti-inflammatory response. Pharmacological activation of PGC1α-IL10 axis may be promising for the treatment of fatty liver diseases. more...

Published

2019

20. SIRT6 Controls Hematopoietic Stem Cell Homeostasis through Epigenetic Regulation of Wnt Signaling

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Author

Xudong Zhu, You Wu, K. Lenhard Rudolph, Zhencan Shi, Shaorong Gao, Guang-Hui Liu, Tangliang Li, Daojun Diao, Yawei Gao, Xiaoyu Liu, Hu Wang, and Zhenyu Ju

Subjects

0301 basic medicine, Biology, Epigenesis, Genetic, Mice, 03 medical and health sciences, Genetics, Animals, Homeostasis, Sirtuins, Epigenetics, Wnt Signaling Pathway, Transcription factor, Hematopoietic stem cell homeostasis, Wnt signaling pathway, LRP6, LRP5, Cell Biology, Hematopoietic Stem Cells, Cell biology, Mice, Inbred C57BL, Wnt Proteins, 030104 developmental biology, Commentary, Molecular Medicine, Histone deacetylase, Adult stem cell

Abstract

Proper regulation of Wnt signaling is critical for the maintenance of hematopoietic stem cell (HSC) homeostasis. The epigenetic regulation of Wnt signaling in HSCs remains largely unknown. Here, we report that the histone deacetylase SIRT6 regulates HSC homeostasis through the transcriptional repression of Wnt target genes. Sirt6 deletion promoted HSC proliferation through aberrant activation of Wnt signaling. SIRT6-deficient HSCs exhibited impaired self-renewal ability in serial competitive transplantation assay. Mechanistically, SIRT6 inhibits the transcription of Wnt target genes by interacting with transcription factor LEF1 and deacetylating histone 3 at lysine 56. Pharmacological inhibition of the Wnt pathway rescued the aberrant proliferation and functional defect in SIRT6-deficient HSCs. Taken together, these findings disclose a new link between SIRT6 and Wnt signaling in the regulation of adult stem cell homeostasis and self-renewal capacity. more...

Published

2016

21. Telomeric epigenetic response mediated by Gadd45a regulates stem cell aging and lifespan

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Author

Zhangfa Song, Zhencan Shi, Xudong Zhu, Daojun Diao, Xiaoqing Jin, Fan Yang, Jing Yan, Yu-Sheng Cong, Tangliang Li, Hu Wang, Tobias Sperka, Zhenyu Ju, Meimei Zhang, Li Shen, and Qimin Zhan

Subjects

0301 basic medicine, Aging, DNA damage, Cell Cycle Proteins, Biology, Biochemistry, Epigenesis, Genetic, Mice, 03 medical and health sciences, Genetics, Animals, Epigenetics, Intestinal Mucosa, Telomerase, Molecular Biology, Mice, Knockout, Stem Cells, Nuclear Proteins, Articles, Base excision repair, Telomere, Chromatin, Cell biology, body regions, 030104 developmental biology, CpG site, RNA, CpG Islands, Stem cell, DNA Damage, Adult stem cell

Abstract

Progressive attrition of telomeres triggers DNA damage response (DDR) and limits the regenerative capacity of adult stem cells during mammalian aging. Intriguingly, telomere integrity is not only determined by telomere length but also by the epigenetic status of telomeric/sub‐telomeric regions. However, the functional interplay between DDR induced by telomere shortening and epigenetic modifications in aging remains unclear. Here, we show that deletion of Gadd45a improves the maintenance and function of intestinal stem cells (ISCs) and prolongs lifespan of telomerase‐deficient mice (G3 Terc −/− ). Mechanistically, Gadd45a facilitates the generation of a permissive chromatin state for DDR signaling by inducing base excision repair‐dependent demethylation of CpG islands specifically at sub‐telomeric regions of short telomeres. Deletion of Gadd45a promotes chromatin compaction in sub‐telomeric regions and attenuates DDR initiation at short telomeres of G3 Terc −/− ISCs. Treatment with a small molecule inhibitor of base excision repair reduces DDR and improves the maintenance and function of G3 Terc −/− ISCs. Taken together, our study proposes a therapeutic approach to enhance stem cell function and prolong lifespan by targeting epigenetic modifiers. more...

Published

2018

22. Smg6/Est1 licenses embryonic stem cell differentiation via nonsense‐mediated <scp>mRNA</scp> decay

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Author

Zhao-Qi Wang, Bao-Fa Sun, Tangliang Li, Pei Wang, Luis Miguel Guachalla, Yun-Gui Yang, Yu-Sheng Chen, Anja Krueger, Karl Lenhard Rudolph, Matthias Platzer, Yue Shi, Tjard Joerss, and Marco Groth

Subjects

Telomerase, Somatic cell, Cellular differentiation, Immunoblotting, Nonsense-mediated decay, Smg6/Est1, Protein Serine-Threonine Kinases, Biology, Real-Time Polymerase Chain Reaction, General Biochemistry, Genetics and Molecular Biology, cell reprograming, Mice, NMD, Animals, ESC differentiation, telomere, Cloning, Molecular, RNA, Small Interfering, Induced pluripotent stem cell, Molecular Biology, Embryonic Stem Cells, In Situ Hybridization, Fluorescence, Tissue homeostasis, DNA Primers, Mice, Knockout, General Immunology and Microbiology, Sequence Analysis, RNA, General Neuroscience, Histological Techniques, Computational Biology, Gene Expression Regulation, Developmental, Cell Differentiation, Articles, Molecular biology, Embryonic stem cell, Nonsense Mediated mRNA Decay, Telomere, Cell biology, Have You Seen?

Abstract

Nonsense-mediated mRNA decay (NMD) is a post-transcriptional mechanism that targets aberrant transcripts and regulates the cellular RNA reservoir. Genetic modulation in vertebrates suggests that NMD is critical for cellular and tissue homeostasis, although the underlying mechanism remains elusive. Here, we generate knockout mice lacking Smg6/Est1, a key nuclease in NMD and a telomerase cofactor. While the complete loss of Smg6 causes mouse lethality at the blastocyst stage, inducible deletion of Smg6 is compatible with embryonic stem cell (ESC) proliferation despite the absence of telomere maintenance and functional NMD. Differentiation of Smg6-deficient ESCs is blocked due to sustained expression of pluripotency genes, normally repressed by NMD, and forced down-regulation of one such target, c-Myc, relieves the differentiation block. Smg6-null embryonic fibroblasts are viable as well, but are refractory to cellular reprograming into induced pluripotent stem cells (iPSCs). Finally, depletion of all major NMD factors compromises ESC differentiation, thus identifying NMD as a licensing factor for the switch of cell identity in the process of stem cell differentiation and somatic cell reprograming. more...

Published

2015

23. Point mutation at the Nbs1 Threonine 278 site does not affect mouse development, but compromises the Chk2 and Smc1 phosphorylation after DNA damage

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Author

Zhao-Qi Wang and Tangliang Li

Subjects

Threonine, Aging, Chromosomal Proteins, Non-Histone, DNA damage, Mutant, Cell Cycle Proteins, Protein Serine-Threonine Kinases, Biology, medicine.disease_cause, environment and public health, Serine, Mice, medicine, Animals, Humans, Point Mutation, Phosphorylation, Mutation, Point mutation, Nuclear Proteins, Dose-Response Relationship, Radiation, medicine.disease, Mice, Mutant Strains, Cell biology, DNA-Binding Proteins, Checkpoint Kinase 2, enzymes and coenzymes (carbohydrates), Biochemistry, Gamma Rays, Nijmegen breakage syndrome, DNA Damage, Developmental Biology

Abstract

NBS1, mutated in Nijmegen breakage syndrome (NBS), senses the DNA double strand breaks (DSBs) and initiates the DNA damage response (DDR) by activating ATM kinase. Meanwhile, NBS1 is phosphorylated by ATM at Serine 278 and Serine 343 and thereby assists the activation of the ATM downstream targets. To study the physiological function of the Nbs1 phosphorylation, we have knocked in a point mutation in the moue genome that results in the replacement of Threonine 278 (equivalent to the human Serine 278) by Alanine. The Nbs1(T278A) knock-in mice develop normally and show no gross defects. The mutation of this phosphorylation site does not affect the proliferation or genomic stability. Ionizing radiation (IR) of primary Nbs1(T278A) MEFs reveals no obvious defects in the Chk2 phosphorylation at 1Gy, but a delayed phosphorylation of Chk2 and Smc1 only at intermediate (4.5Gy) and high (10Gy) doses, respectively. In contrast to Serine 343 mutant, Threonine 278 mutation has no effect on the HU-induced ATR-Chk1 activation. Our study thus shows that Nbs1 phosphorylation at the Threonine 278 is dispensable for mouse development and plays a differential function in assisting the DDR of downstream effectors in vivo, depending on the doses of DNA damage. more...

Published

2011

24. The E3 ubiquitin ligase APC/C

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Author

Xiaoqian, Liu, Wen, Zong, Tangliang, Li, Yujun, Wang, Xingzhi, Xu, Zhong-Wei, Zhou, and Zhao-Qi, Wang

Subjects

Neurogenesis, Ubiquitin-Protein Ligases, Mitosis, Cell Cycle Proteins, Cell Differentiation, Nerve Tissue Proteins, Articles, beta-Transducin Repeat-Containing Proteins, Cell Line, Cytoskeletal Proteins, Gene Knockout Techniques, Mice, Neural Stem Cells, Two-Hybrid System Techniques, Animals, Homeostasis, Humans, cdc25 Phosphatases, DNA Damage

Abstract

Mutations of microcephalin (MCPH1) can cause the neurodevelopmental disorder primary microcephaly type 1. We previously showed that MCPH1 deletion in neural stem cells results in early mitotic entry that distracts cell division mode, leading to exhaustion of the progenitor pool. Here, we show that MCPH1 interacts with and promotes the E3 ligase βTrCP2 to degrade Cdc25A independent of DNA damage. Overexpression of βTrCP2 or the knockdown of Cdc25A remedies the high mitotic index and rescues the premature differentiation of Mcph1‐deficient neuroprogenitors in vivo. MCPH1 itself is degraded by APC/CC dh1, but not APC/CC dc20, in late mitosis and G1 phase. Forced MCPH1 expression causes cell death, underlining the importance of MCPH1 turnover after mitosis. Ectopic expression of Cdh1 leads to premature differentiation of neuroprogenitors, mimicking differentiation defects of Mcph1‐knockout neuroprogenitors. The homeostasis of MCPH1 in association with the ubiquitin‐proteasome system ensures mitotic entry independent of cell cycle checkpoint. This study provides a mechanistic understanding of how MCPH1 controls neural stem cell fate and brain development. more...

Published

2016

25. Reciprocal chromosome painting between three laboratory rodent species

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Author

Roscoe Stanyon, Vladimir A. Trifonov, Malcolm A. Ferguson-Smith, Fengtang Yang, Tangliang Li, Larisa S. Biltueva, Polina L. Perelman, Wenhui Nie, Svetlana A. Romanenko, V. Volobouev, Natalya A. Serdukova, Alexander S. Graphodatsky, Patricia C. M. O’Brien, and Jinhuan Wang more...

Subjects

Male, animal diseases, Hamster, Chinese hamster, Chromosome Painting, Mice, Cricetulus, Cricetinae, parasitic diseases, Genetics, Animals, Cells, Cultured, In Situ Hybridization, Fluorescence, Genome, Mesocricetus, biology, Laboratory mouse, Chromosome, Karyotype, Physical Chromosome Mapping, biology.organism_classification, Chromosomes, Mammalian, humanities, Karyotyping, Ploidy, DNA Probes, Golden hamster

Abstract

The laboratory mouse (Mus musculus, 2n = 40), the Chinese hamster (Cricetulus griseus, 2n = 22), and the golden (Syrian) hamster (Mesocricetus auratus, 2n = 44) are common laboratory animals, extensively used in biomedical research. In contrast with the mouse genome, which was sequenced and well characterized, the hamster species has been set aside. We constructed a chromosome paint set for the golden hamster, which for the first time allowed us to perform multidirectional chromosome painting between the golden hamster and the mouse and between the two species of hamster. From these data we constructed a detailed comparative chromosome map of the laboratory mouse and the two hamster species. The golden hamster painting probes revealed 25 autosomal segments in the Chinese hamster and 43 in the mouse. Using the Chinese hamster probes, 23 conserved segments were found in the golden hamster karyotype. The mouse probes revealed 42 conserved autosomal segments in the golden hamster karyotype. The two largest chromosomes of the Chinese hamster (1 and 2) are homologous to seven and five chromosomes of the golden hamster, respectively. The golden hamster karyotype can be transformed into the Chinese hamster karyotype by 15 fusions and 3 fissions. Previous reconstructions of the ancestral murid karyotype proposed diploid numbers from 2n = 52 to 2n = 54. By integrating the new multidirectional chromosome painting data presented here with previous comparative genomics data, we can propose that syntenies to mouse Chrs 6 and 16 were both present and to hypothesize a diploid number of 2n = 48 for the ancestral Murinae/Cricetinae karyotype. more...

Published

2006

26. Comparative genome maps of the pangolin, hedgehog, sloth, anteater and human revealed by cross-species chromosome painting: further insight into the ancestral karyotype and genome evolution of eutherian mammals

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Author

Yingxiang Wang, Natalya A. Serdukova, Malcolm A. Ferguson-Smith, J. Wang, Beiyuan Fu, Fengtang Yang, Tangliang Li, Polina L. Perelman, V. Volobouev, Weiting Su, Gauthier Dobigny, Alexander S. Graphodatsky, Wenhui Nie, and Patricia C. M. O’Brien more...

Subjects

Male, Genome evolution, Synteny, Chromosome Painting, Genome diversity and karyotype evolution of mammals, Evolution, Molecular, 03 medical and health sciences, Species Specificity, Convergent evolution, Genetics, Animals, Humans, In Situ Hybridization, Fluorescence, 030304 developmental biology, Mammals, 0303 health sciences, Genome, biology, Genome, Human, 030305 genetics & heredity, Pangolin, Pholidota, Xenarthra, biology.organism_classification, Chromosomes, Mammalian, Hedgehogs, Karyotyping, Cytogenetic Analysis, Female, Afrotheria

Abstract

To better understand the evolution of genome organization of eutherian mammals, comparative maps based on chromosome painting have been constructed between human and representative species of three eutherian orders: Xenarthra, Pholidota, and Eulipotyphla, as well as between representative species of the Carnivora and Pholidota. These maps demonstrate the conservation of such syntenic segment associations as HSA3/21, 4/8, 7/16, 12/22, 14/15 and 16/19 in Eulipotyphla, Pholidota and Xenarthra and thus further consolidate the notion that they form part of the ancestral karyotype of the eutherian mammals. Our study has revealed many potential ancestral syntenic associations of human chromosomal segments that serve to link the families as well as orders within the major superordinial eutherian clades defined by molecular markers. The HSA2/8 and 7/10 associations could be the cytogenetic signatures that unite the Xenarthrans, while the HSA1/19p could be a putative signature that links the Afrotheria and Xenarthra. But caution is required in the interpretation of apparently shared syntenic associations as detailed analyses also show examples of apparent convergent evolution that differ in breakpoints and extent of the involved segments. more...

Published

2006

27. Chromosomal mechanisms underlying the karyotype evolution of the oriental voles (Muridae, Eothenomys)

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Author

Tangliang Li, Fengtang Yang, J. Wang, and W. Su

Subjects

biology, Eothenomys proditor, Genetics, Eothenomys, Zoology, Vole, Karyotype, biology.organism_classification, Eothenomys miletus, Molecular Biology, Genetics (clinical), Muridae

Abstract

We have investigated the karyotype relationships of two oriental voles, i.e. the Yulong vole (Eothenomys proditor, 2n = 32) and the large oriental vole (Eothenomys miletus, 2n = 56) as well as the Clarke’s vole (Microtus clarkei, 2n = 52), by a combined approach of cross-species chromosome painting and high-resolution G-banding comparison. Chromosome-specific painting probes were generated from flow-sorted chromosomes of E. proditor and hybridized onto metaphases of E. proditor, E. miletus and M. clarkei, leading to the establishment of genome-wide comparative chromosome maps. Our results demonstrate that Robertsonian translocations (centric fusions) have played a major role in the karyotype evolution of oriental voles with no obvious evidence for the involvement of tandem fusions as proposed previously and that the genome organizations of vole species are highly conserved. The comparative chromosome maps of these three vole species belonging to two phylogenetically distinct genera provide a framework for future studies on the karyotype evolution in voles. more...

Published

2006

28. Karyotypic evolution of the family Sciuridae: inferences from the genome organizations of ground squirrels

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Author

W. Nie, Fengtang Yang, Tangliang Li, W. Su, and J. Wang

Subjects

Genetics, Painting, Genome, Cell Culture Techniques, Sciuridae, Karyotype, Fibroblasts, Biology, humanities, Chromosome Banding, Chromosome Painting, Genome diversity and karyotype evolution of mammals, Evolution, Molecular, Evolutionary biology, Karyotyping, Animals, Humans, Chromosome painting, FAMILY SCIURIDAE, Molecular Biology, In Situ Hybridization, Fluorescence, Metaphase, Genetics (clinical)

Abstract

Cross-species chromosome painting has made a great contribution to our understanding of the evolution of karyotypes and genome organizations of mammals. Several recent papers of comparative painting between tree and flying squirrels have shed some light on the evolution of the family Sciuridae and the order Rodentia. In the present study we have extended the comparative painting to the Himalayan marmot (Marmotahimalayana) and the African ground squirrel (Xerus cf. erythropus), i.e. representative species from another important squirrel group – the ground squirrels –, and have established genome-wide comparative chromosome maps between human, eastern gray squirrel, and these two ground squirrels. The results show that 1) the squirrels so far studied all have conserved karyotypes that resemble the ancestral karyotype of the order Rodentia; 2) the African ground squirrels could have retained the ancestral karyotype of the family Sciuridae. Furthermore, we have mapped the evolutionary rearrangements onto a molecular-based consensus phylogenetic tree of the family Sciuridae. more...

Published

2006

29. A first generation comparative chromosome map between guinea pig (Cavia porcellus) and humans

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Author

Bee Ling Ng, Patricia C. M. O’Brien, Thomas Liehr, Fengtang Yang, Vladimir A. Trifonov, Wenhui Nie, Roscoe Stanyon, Natalia A. Serdyukova, Polina L. Perelman, Alexander S. Graphodatsky, Beiyuan Fu, Tangliang Li, and Svetlana A. Romanenko more...

Subjects

Genome evolution, Guinea Pigs, Cavia, lcsh:Medicine, Genome, Chromosome Painting, Evolution, Molecular, Guinea pig, 03 medical and health sciences, Species Specificity, Animals, Chromosomes, Human, Humans, Agricultural and Biological Sciences (all), Biochemistry, Genetics and Molecular Biology (all), Medicine (all), lcsh:Science, 030304 developmental biology, Synteny, Genetics, 0303 health sciences, Multidisciplinary, biology, Gene map, Genome, Human, 030305 genetics & heredity, lcsh:R, Chromosome Mapping, Chromosome, Karyotype, biology.organism_classification, lcsh:Q, Research Article

Abstract

The domesticated guinea pig, Cavia porcellus (Hystricomorpha, Rodentia), is an important laboratory species and a model for a number of human diseases. Nevertheless, genomic tools for this species are lacking; even its karyotype is poorly characterized. The guinea pig belongs to Hystricomorpha, a widespread and important group of rodents; so far the chromosomes of guinea pigs have not been compared with that of other hystricomorph species or with any other mammals. We generated full sets of chromosome-specific painting probes for the guinea pig by flow sorting and microdissection, and for the first time, mapped the chromosomal homologies between guinea pig and human by reciprocal chromosome painting. Our data demonstrate that the guinea pig karyotype has undergone extensive rearrangements: 78 synteny-conserved human autosomal segments were delimited in the guinea pig genome. The high rate of genome evolution in the guinea pig may explain why the HSA7/16 and HSA16/19 associations presumed ancestral for eutherians and the three syntenic associations (HSA1/10, 3/19, and 9/11) considered ancestral for rodents were not found in C. porcellus. The comparative chromosome map presented here is a starting point for further development of physical and genetic maps of the guinea pig as well as an aid for genome assembly assignment to specific chromosomes. Furthermore, the comparative mapping will allow a transfer of gene map data from other species. The probes developed here provide a genomic toolkit, which will make the guinea pig a key species to unravel the evolutionary biology of the Hystricomorph rodents. more...

Published

2015

30. An essential function for the ATR-activation-domain (AAD) of TopBP1 in mouse development and cellular senescence

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Author

Anja Krueger, Christopher Bruhn, Zhao-Qi Wang, Wookee Min, Tangliang Li, Zhong-Wei Zhou, Antony M. Carr, and Cong Liu

Subjects

Cancer Research, lcsh:QH426-470, Embryonic Development, Ataxia Telangiectasia Mutated Proteins, Biology, Mice, 03 medical and health sciences, Genetics, Animals, Point Mutation, Gene Knock-In Techniques, CHEK1, Phosphorylation, Molecular Biology, Alleles, Cellular Senescence, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, Cell Proliferation, 030304 developmental biology, QD0415, 0303 health sciences, Cell growth, Activator (genetics), 030302 biochemistry & molecular biology, Wild type, Gene Expression Regulation, Developmental, Molecular biology, Protein Structure, Tertiary, Cell biology, lcsh:Genetics, Checkpoint Kinase 1, Signal transduction, biological phenomena, cell phenomena, and immunity, Carrier Proteins, Protein Kinases, Cell aging, Signal Transduction, Research Article

Abstract

ATR activation is dependent on temporal and spatial interactions with partner proteins. In the budding yeast model, three proteins – Dpb11TopBP1, Ddc1Rad9 and Dna2 - all interact with and activate Mec1ATR. Each contains an ATR activation domain (ADD) that interacts directly with the Mec1ATR:Ddc2ATRIP complex. Any of the Dpb11TopBP1, Ddc1Rad9 or Dna2 ADDs is sufficient to activate Mec1ATR in vitro. All three can also independently activate Mec1ATR in vivo: the checkpoint is lost only when all three AADs are absent. In metazoans, only TopBP1 has been identified as a direct ATR activator. Depletion-replacement approaches suggest the TopBP1-AAD is both sufficient and necessary for ATR activation. The physiological function of the TopBP1 AAD is, however, unknown. We created a knock-in point mutation (W1147R) that ablates mouse TopBP1-AAD function. TopBP1-W1147R is early embryonic lethal. To analyse TopBP1-W1147R cellular function in vivo, we silenced the wild type TopBP1 allele in heterozygous MEFs. AAD inactivation impaired cell proliferation, promoted premature senescence and compromised Chk1 signalling following UV irradiation. We also show enforced TopBP1 dimerization promotes ATR-dependent Chk1 phosphorylation. Our data suggest that, unlike the yeast models, the TopBP1-AAD is the major activator of ATR, sustaining cell proliferation and embryonic development., Author Summary DNA damage checkpoint signalling is an essential component of the DNA damage response. Many of the key proteins initiating the checkpoint signal have been identified and characterised in yeast. Here we explore the role of the ATR activating domain (AAD) of TopBP1 in embryonic development, cell growth and checkpoint activation using a mouse model. In contrast to yeasts, where the TopBP1 AAD plays a redundant, and thus phenotypically minor, role in ATR activation, our data demonstrate that the mouse TopBP1 AAD is essential for cellular proliferation. Interestingly, this suggests evolution has provided a simpler ATR activation mechanism in metazoans than it has in yeasts. more...

Published

2013

31. Dual Functions of Nbs1 in the Repair of DNA Breaks and Proliferation Ensure Proper V(D)J Recombination and T-Cell Development

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Author

Falk Weih, Patrick Concannon, Tangliang Li, Zhao-Qi Wang, and Amal Saidi

Subjects

DNA Repair, Genes, Immunoglobulin Heavy Chain, T-Lymphocytes, T cell, Cell Cycle Proteins, Biology, Mice, chemistry.chemical_compound, Lymphopenia, medicine, Animals, Humans, Gene Rearrangement, beta-Chain T-Cell Antigen Receptor, Nijmegen Breakage Syndrome, Molecular Biology, Cell Proliferation, DNA Primers, Mice, Knockout, Recombination, Genetic, Base Sequence, DNA Breaks, V(D)J recombination, T-cell receptor, Nuclear Proteins, Cell Differentiation, Articles, Cell Biology, Genes, p53, medicine.disease, Molecular biology, DNA-Binding Proteins, Disease Models, Animal, medicine.anatomical_structure, chemistry, Rad50, Mutation, Ectopic expression, Gene Rearrangement, alpha-Chain T-Cell Antigen Receptor, Chromatin immunoprecipitation, Nijmegen breakage syndrome, DNA

Abstract

Immunodeficiency and lymphoid malignancy are hallmarks of the human disease Nijmegen breakage syndrome (NBS; OMIM 251260), which is caused by NBS1 mutations. Although NBS1 has been shown to bind to the T-cell receptor alpha (TCRα) locus, its role in TCRβ rearrangement is unclear. Hypomorphic mutations of Nbs1 in mice and patients result in relatively mild T-cell deficiencies, raising the question of whether the truncated Nbs1 protein might have clouded a certain function of NBS1 in T-cell development. Here we show that the deletion of the entire Nbs1 protein in T-cell precursors (Nbs1 T-del) results in severe lymphopenia and a hindrance to the double-negative 3 (DN3)-to-DN4 transition in early T-cell development, due to abnormal TCRβ coding and signal joints as well as the functions of Nbs1 in T-cell expansion. Chromatin immunoprecipitation (ChIP) analysis of the TCR loci reveals that Nbs1 depletion compromises the loading of Mre11/ Rad50 to V(D)J-generated DNA double-strand breaks (DSBs) and thereby affects resection of DNA termini and chromatin conformation of the postcleavage complex. Although a p53 deficiency relieves the DN3→DN4 transition block, neither a p53 deficiency nor ectopic expression of TCRαβ rescues the major T-cell loss in Nbs1T-del mice. All together, these results demonstrate that Nbs1's functions in both repair of V(D)J-generated DSBs and proliferation are essential for T-cell development. Copyright © 2010, American Society for Microbiology. All Rights Reserved. more...

Published

2010

32. Evolution of genome organizations of squirrels (Sciuridae) revealed by cross-species chromosome painting

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Author

Malcolm A. Ferguson-Smith, Jinhuan Wang, Beiyuan Fu, Alexander S. Graphodatsky, Wenhui Nie, Larisa S. Biltueva, Patricia C. M. O’Brien, Tangliang Li, and Fengtang Yang

Subjects

Petaurista, Sciurus carolinensis, Genome, Phylogenetic tree, Zoology, Glires, Sciuridae, Karyotype, Biology, biology.organism_classification, Biological Evolution, Chromosomes, Chromosome Banding, Chromosome Painting, Rats, Mice, Karyotyping, Genetics, Animals, Rabbits, Callosciurus erythraeus, Phylogeny, Synteny, Sciurus

Abstract

With complete sets of chromosome-specific painting probes derived from flow-sorted chromosomes of human and grey squirrel (Sciurus carolinensis), the whole genome homologies between human and representatives of tree squirrels (Sciurus carolinensis, Callosciurus erythraeus), flying squirrels (Petaurista albiventer) and chipmunks (Tamias sibiricus) have been defined by cross-species chromosome painting. The results show that, unlike the highly rearranged karyotypes of mouse and rat, the karyotypes of squirrels are highly conserved. Two methods have been used to reconstruct the genome phylogeny of squirrels with the laboratory rabbit (Oryctolagus cuniculus) as the out-group: (1) phylogenetic analysis by parsimony using chromosomal characters identified by comparative cytogenetic approaches; (2) mapping the genome rearrangements onto recently published sequence-based molecular trees. Our chromosome painting results, in combination with molecular data, show that flying squirrels are phylogenetically close to New World tree squirrels. Chromosome painting and G-banding comparisons place chipmunks (Tamias sibiricus ), with a derived karyotype, outside the clade comprising tree and flying squirrels. The superorder Glires (orde Rodentia + order Lagomorpha) is firmly supported by two conserved syntenic associations between human chromosomes 1 and 10p homologues, and between 9 and 11 homologues. more...

Published

2004

33. Reciprocal chromosome painting between three laboratory rodent species.

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Author

Romanenko, Svetlana A., Perelman, Polina L., Serdukova, Natalya A., Trifonov, Vladimir A., Biltueva, Larisa S., Jinhuan ang, Tangliang Li, Wenhui Nie, O'Brien, Patricia C. M., Volobouev, Vitaly T., Stanyon, Roscoe, Ferguson-Smith, Malcolm A., Fengtang Yang, and Graphodatsky, Alexander S. more...

Subjects

CHROMOSOMES, LABORATORY rodents, HAMSTERS, MEDICAL research, GENOMES, KARYOTYPES, FORMALDEHYDE, MICROSCOPY

Abstract

The laboratory mouse ( Mus musculus, 2 n = 40), the Chinese hamster (Cricetulus griseus, 2 n = 22), and the golden (Syrian) hamster ( Mesocricetus auratus, 2 n = 44) are common laboratory animals, extensively used in biomedical research. In contrast with the mouse genome, which was sequenced and well characterized, the hamster species has been set aside. We constructed a chromosome paint set for the golden hamster, which for the first time allowed us to perform multidirectional chromosome painting between the golden hamster and the mouse and between the two species of hamster. From these data we constructed a detailed comparative chromosome map of the laboratory mouse and the two hamster species. The golden hamster painting probes revealed 25 autosomal segments in the Chinese hamster and 43 in the mouse. Using the Chinese hamster probes, 23 conserved segments were found in the golden hamster karyotype. The mouse probes revealed 42 conserved autosomal segments in the golden hamster karyotype. The two largest chromosomes of the Chinese hamster (1 and 2) are homologous to seven and five chromosomes of the golden hamster, respectively. The golden hamster karyotype can be transformed into the Chinese hamster karyotype by 15 fusions and 3 fissions. Previous reconstructions of the ancestral murid karyotype proposed diploid numbers from 2 n = 52 to 2 n = 54. By integrating the new multidirectional chromosome painting data presented here with previous comparative genomics data, we can propose that syntenies to mouse Chrs 6 and 16 were both present and to hypothesize a diploid number of 2 n = 48 for the ancestral Murinae/Cricetinae karyotype. [ABSTRACT FROM AUTHOR] more...

Published

2006

34. Comparative genome maps of the pangolin, hedgehog, sloth, anteater and human revealed by cross-species chromosome painting: further insight into the ancestral karyotype and genome evolution of eutherian mammals.

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Author

Fengtang Yang, Alexander Graphodatsky, Tangliang Li, Beiyuan Fu, Gauthier Dobigny, Jinghuan Wang, Polina Perelman, Natalya Serdukova, Weiting Su, Patricia O'Brien, Yingxiang Wang, Malcolm Ferguson-Smith, Vitaly Volobouev, and Wenhui Nie more...

Abstract

To better understand the evolution of genome organization of eutherian mammals, comparative maps based on chromosome painting have been constructed between human and representative species of three eutherian orders: Xenarthra, Pholidota, and Eulipotyphla, as well as between representative species of the Carnivora and Pholidota. These maps demonstrate the conservation of such syntenic segment associations as HSA3/21, 4/8, 7/16, 12/22, 14/15 and 16/19 in Eulipotyphla, Pholidota and Xenarthra and thus further consolidate the notion that they form part of the ancestral karyotype of the eutherian mammals. Our study has revealed many potential ancestral syntenic associations of human chromosomal segments that serve to link the families as well as orders within the major superordinial eutherian clades defined by molecular markers. The HSA2/8 and 7/10 associations could be the cytogenetic signatures that unite the Xenarthrans, while the HSA1/19p could be a putative signature that links the Afrotheria and Xenarthra. But caution is required in the interpretation of apparently shared syntenic associations as detailed analyses also show examples of apparent convergent evolution that differ in breakpoints and extent of the involved segments. [ABSTRACT FROM AUTHOR] more...

Published

2006

35. Evolution of Genome Organizations of Squirrels (Sciuridae) Revealed by Cross-Species Chromosome Painting.

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Author

Tangliang Li, Patricia C. M. O'Brien, Larisa Biltueva, Beiyuan Fu, and Jinhuan Wang

Abstract

With complete sets of chromosome-specific painting probes derived from flow-sorted chromosomes of human and grey squirrel (Sciurus carolinensis), the whole genome homologies between human and representatives of tree squirrels (Sciurus carolinensis, Callosciurus erythraeus), flying squirrels (Petaurista albiventer) and chipmunks (Tamias sibiricus) have been defined by cross-species chromosome painting. The results show that, unlike the highly rearranged karyotypes of mouse and rat, the karyotypes of squirrels are highly conserved. Two methods have been used to reconstruct the genome phylogeny of squirrels with the laboratory rabbit (Oryctolagus cuniculus) as the out-group: (1) phylogenetic analysis by parsimony using chromosomal characters identified by comparative cytogenetic approaches; (2) mapping the genome rearrangements onto recently published sequence-based molecular trees. Our chromosome painting results, in combination with molecular data, show that flying squirrels are phylogenetically close to New World tree squirrels. Chromosome painting and G-banding comparisons place chipmunks (Tamias sibiricus), with a derived karyotype, outside the clade comprising tree and flying squirrels. The superorder Glires (orde Rodentia + order Lagomorpha) is firmly supported by two conserved syntenic associations between human chromosomes 1 and 10p homologues, and between 9 and 11 homologues. [ABSTRACT FROM AUTHOR] more...

Published

2004

36. Dual Functions of Nbs1 in the Repair of DNA Breaks and Proliferation Ensure Proper V(D)J Recombination and T-Cell Development.

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Author

Saidi, Amal, Tangliang Li, Weih, Falk, Concannon, Patrick, and Zhao-Qi Wang

Subjects

*IMMUNODEFICIENCY, *LYMPHOID tissue, *GENETIC mutation, *T cell receptors, *LYMPHOPENIA, *CHROMATIN, *CANCER

Abstract

Immunodeficiency and lymphoid malignancy are hallmarks of the human disease Nijmegen breakage syndrome (NBS; OMIM 251260), which is caused by NBS1 mutations. Although NBS1 has been shown to bind to the T-cell receptor alpha (TCRα) locus, its role in TCRβ rearrangement is unclear. Hypomorphic mutations of Nbs1 in mice and patients result in relatively mild T-cell deficiencies, raising the question of whether the truncated Nbs1 protein might have clouded a certain function of NBS1 in T-cell development. Here we show that the deletion of the entire Nbs1 protein in T-cell precursors (Nbs1T-del) results in severe lymphopenia and a hindrance to the double-negative 3 (DN3)-to-DN4 transition in early T-cell development, due to abnormal TCRβ coding and signal joints as well as the functions of Nbs1 in T-cell expansion. Chromatin immunoprecipitation (ChIP) analysis of the TCR loci reveals that Nbs1 depletion compromises the loading of Mre11/Rad50 to V(D)J-generated DNA double-strand breaks (DSBs) and thereby affects resection of DNA termini and chromatin conformation of the postcleavage complex. Although a p53 deficiency relieves the DN3→DN4 transition block, neither a p53 deficiency nor ectopic expression of TCRαβ rescues the major T-cell loss in Nbs1T-del mice. All together, these results demonstrate that Nbs1's functions in both repair of V(D)J-generated DSBs and proliferation are essential for T-cell development. [ABSTRACT FROM AUTHOR] more...

Published

2010