Your search keyword '"van Deursen, Jan M"' showing total 7 results

1. BubR1 allelic effects drive phenotypic heterogeneity in mosaic-variegated aneuploidy progeria syndrome

Author

Sieben, Cynthia J., Jeganathan, Karthik B., Nelson, Grace G., Sturmlechner, Ines, Zhang, Cheng, van Deursen, Willemijn H., Bakker, Bjorn, Foijer, Floris, Li, Hu, Baker, Darren J., and van Deursen, Jan M.

Subjects

Birth defects, Skeletal muscle, Medical research, Genetic disorders, Progeria, Childhood, Cancer, Dwarfism, Phenotypes, Diseases, Hyperactivity, Sarcopenia, Lipodystrophy, Health care industry, Gene Ontology. Gene Ontology Consortium

Abstract

Mosaic-variegated aneuploidy (MVA) syndrome is a rare childhood disorder characterized by biallelic BUBR1, CEP57, or TRIP13 aberrations; increased chromosome missegregation; and a broad spectrum of clinical features, including various cancers, congenital defects, and progeroid pathologies. To investigate the mechanisms underlying this disorder and its phenotypic heterogeneity, we mimicked the [BUBR1.sup.L1012P] mutation in mice ([BubR1.sup.L1002P]) and combined it with 2 other MVA variants, [BUBR1.sup.X753] and [BUBR1.sup.H], generating a truncated protein and low amounts of wild-type protein, respectively. Whereas [BubR1.sup.X753/L1002P] and [BubR1.sup.H/X753] mice died prematurely, [BubR1.sup.H/L1002P] mice were viable and exhibited many MVA features, including cancer predisposition and various progeroid phenotypes, such as short lifespan, dwarfism, lipodystrophy, sarcopenia, and low cardiac stress tolerance. Strikingly, although these mice had a reduction in total BUBR1 and spectrum of MVA phenotypes similar to that of [BubR1.sup.H/H] mice, several progeroid pathologies were attenuated in severity, which in skeletal muscle coincided with reduced senescence-associated secretory phenotype complexity. Additionally, mice carrying monoallelic BubRI mutations were prone to select MVA-related pathologies later in life, with predisposition to sarcopenia correlating with mTORC1 hyperactivity. Together, these data demonstrate that BUBR1 allelic effects beyond protein level and aneuploidy contribute to disease heterogeneity in both MVA patients and heterozygous carriers of MVA mutations., Introduction Mosaic-variegated aneuploidy (MVA) syndrome is an autosomal recessive syndrome characterized by near-diploid aneuploidies involving multiple tissues and chromosomes (1-4). A wide variety of additional clinical features are associated with [...]

Published

2020

2. Mosaic-variegated aneuploidy syndrome mutation or haploinsufficiency in Cep57 impairs tumor suppression

Author

Aziz, Khaled, Sieben, Cynthia J., Jeganathan, Karthik B., Hamada, Masakazu, Davies, Brian A., Velasco, Raul O. Fierro, Rahman, Nazneen, Katzmann, David J., and van Deursen, Jan M.

Subjects

Osteoblasts -- Analysis, Gene mutation -- Research, Aneuploidy -- Genetic aspects -- Models -- Development and progression -- Research, Fibroblasts -- Analysis, Health care industry

Abstract

A homozygous truncating frameshift mutation in CEP57([CEP57.sup.T/T]) has been identified in a subset of mosaic- variegated aneuploidy (MVA) patients; however, the physiological roles of the centrosome- associated protein CEP57 that contribute to disease are unknown. To investigate these, we have generated a mouse model mimicking this disease mutation. [Cep57.sup.T/T] mice died within 24 hours after birth with short, curly tails and severely impaired vertebral ossification. Osteoblasts in lumbosacral vertebrae of [Cep57.sup.T/T] mice were deficient for Fgf2, a Cep57 binding partner implicated in diverse biological processes, including bone formation. Furthermore, a broad spectrum of tissues of [CEP57.sup.T/T] mice had severe aneuploidy at birth, consistent with the MVA patient phenotype. [Cep57.sup.T/T] mouse embryonic fibroblasts and patient-derived skin fibroblasts failed to undergo centrosome maturation in [G.sub.2] phase, causing premature centriole disjunction, centrosome amplification, aberrant spindle formation, and high rates of chromosome missegregation. Mice heterozygous for the truncating frameshift mutation or a Cep57-null allele were overtly indistinguishable from WT mice despite reduced Cep57 protein levels, yet prone to aneuploidization and cancer, with tumors lacking evidence for loss of heterozygosity. This study identifies Cep57 as a haploinsufficient tumor suppressor with biologically diverse roles in centrosome maturation and Fgf2-mediated bone formation., Introduction Rare hereditary human syndromes characterized by extensive genetic and phenotypic heterogeneity are among the most difficult diseases to understand at a molecular mechanistic level, and research on such syndromes [...]

Published

2018

3. Senescent cells: a therapeutic target for cardiovascular disease

Author

Childs, Bennett G., Li, Hu, and van Deursen, Jan M.

Subjects

Cardiovascular diseases -- Prevention -- Health aspects -- Risk factors -- Development and progression -- Care and treatment, Cell aging -- Health aspects -- Models, Health care industry

Abstract

Cellular senescence, a major tumor-suppressive cell fate, has emerged from humble beginnings as an in vitro phenomenon into recognition as a fundamental mechanism of aging. In the process, senescent cells have attracted attention as a therapeutic target for age-related diseases, including cardiovascular disease (CVD), the leading cause of morbidity and mortality in the elderly. Given the aging global population and the inadequacy of current medical management, attenuating the health care burden of CVD would be transformative to clinical practice. Here, we review the evidence that cellular senescence drives CVD in a bimodal fashion by both priming the aged cardiovascular system for disease and driving established disease forward. Hence, the growing field of senotherapy (neutralizing senescent cells for therapeutic benefit) is poised to contribute to both prevention and treatment of CVD., Introduction During aging, the human mortality rate rises exponentially as a result of a loss of normal organ functions, including tissue maintenance and repair capacity. Stressors that young tissue may [...]

Published

2018

4. Nuclear pore protein NUP88 activates anaphase-promoting complex to promote aneuploidy

Author

Naylor, Ryan M., Jeganathan, Karthik B., Cao, Xiuqi, and van Deursen, Jan M.

Subjects

Gene expression -- Health aspects, Carcinogenesis -- Genetic aspects, Aneuploidy -- Identification and classification, Cellular proteins -- Properties, Health care industry

Abstract

The nuclear pore complex protein NUP88 is frequently elevated in aggressive human cancers and correlates with reduced patient survival; however, it is unclear whether and how NUP88 overexpression drives tumorigenesis. Here, we show that mice overexpressing NUP88 are cancer prone and form intestinal tumors. To determine whether overexpression of NUP88 drives tumorigenesis, we engineered transgenic mice with doxycycline-inducible expression of Nup88. Surprisingly, NUP88 overexpression did not alter global nuclear transport, but was a potent inducer of aneuploidy and chromosomal instability. We determined that NUP88 and the nuclear transport factors NUP98 and RAE1 comprise a regulatory network that inhibits premitotic activity of the anaphase-promoting complex/cyclosome (APC/C). When overexpressed, NUP88 sequesters NUP98-RAE1 away from [APC/C.sup.CDH1], triggering proteolysis of polo-like kinase 1 (PLK1), a tumor suppressor and multitasking mitotic kinase. Premitotic destruction of PLK1 disrupts centrosome separation, causing mitotic spindle asymmetry, merotelic microtubule-kinetochore attachments, lagging chromosomes, and aneuploidy. These effects were replicated by PLK1 insufficiency, indicating that PLK1 is responsible for the mitotic defects associated with NUP88 overexpression. These findings demonstrate that the NUP88-NUP98-RAE1-[APC/C.sup.CDH1] axis contributes to aneuploidy and suggest that it may be deregulated in the initiating stages of a broad spectrum of human cancers., Introduction Nuclear pore complexes (NPCs) are channels embedded in the nuclear envelope (NE) that facilitate trafficking of macromolecules into and out of the nucleus (1). The NPC consists of approximately [...]

Published

2016

5. Histone demethylase JMJD2A drives prostate tumorigenesis through transcription factor ETV1

Author

Kim, Tae-Dong, Jin, Fang, Shin, Sook, Oh, Sangphil, Lightfoot, Stan A., Grande, Joseph P., Johnson, Aaron J., van Deursen, Jan M., Wren, Jonathan D., and Janknecht, Ralf

Subjects

Prostate cancer -- Genetic aspects -- Development and progression, Genetic transcription -- Health aspects, Oxidoreductases -- Health aspects, Transcription factors -- Properties, Health care industry

Abstract

Histone demethylase upregulation has been observed in human cancers, yet it is unknown whether this is a bystander event or a driver of tumorigenesis. We found that overexpression of lysine-specific demethylase 4A (KDM4A, also known as JMJD2A) was positively correlated with Gleason score and metastasis in human prostate tumors. Overexpression of JMJD2A resulted in the development of prostatic intraepithelial neoplasia in mice, demonstrating that JMJD2A can initiate prostate cancer development. Moreover, combined overexpression of JMJD2A and the ETS transcription factor ETV1, a JMJD2A-binding protein, resulted in prostate carcinoma formation in mice haplodeficient for the phosphatase and tensin homolog (Pten) tumor-suppressor gene. Additionally, JMJD2A cooperated with ETV1 to increase expression of yes associated protein 1 (YAP1), a Hippo pathway component that itself was associated with prostate tumor aggressiveness. ETV1 facilitated the recruitment of JMJD2A to the YAP1 promoter, leading to changes in histone lysine methylation in a human prostate cancer cell line. Further, YAP1 expression largely rescued the growth inhibitory effects of JMJD2A depletion in prostate cancer cells, indicating that YAP1 is a downstream effector of JMJD2A. Taken together, these data reveal a JMJD2A/ETV1/YAP1 axis that promotes prostate cancer initiation and that may be a suitable target for therapeutic inhibition., Introduction Prostate tumors are the most frequently diagnosed cancer in US men and a major health problem throughout the world. Apart from surgery and radiotherapy, androgen ablation is a standard [...]

Published

2016

6. BubR1 allelic effects drive phenotypic heterogeneity in mosaic-variegated aneuploidy progeria syndrome

Author

Sieben, Cynthia J., primary, Jeganathan, Karthik B., additional, Nelson, Grace G., additional, Sturmlechner, Ines, additional, Zhang, Cheng, additional, van Deursen, Willemijn H., additional, Bakker, Bjorn, additional, Foijer, Floris, additional, Li, Hu, additional, Baker, Darren J., additional, and van Deursen, Jan M., additional

Published

2019

7. Histone demethylase JMJD2A drives prostate tumorigenesis through transcription factor ETV1.

Author

Tae-Dong Kim, Fang Jin, Sook Shin, Sangphil Oh, Lightfoot, Stan A., Grande, Joseph P., Johnson, Aaron J., van Deursen, Jan M., Wren, Jonathan D., Janknecht, Ralf, Kim, Tae-Dong, Jin, Fang, Shin, Sook, and Oh, Sangphil

Subjects

*PROSTATE tumors, *HISTONE demethylases, *NEOPLASTIC cell transformation, *TRANSCRIPTION factors, *GENETIC overexpression, *LABORATORY mice

Abstract

Histone demethylase upregulation has been observed in human cancers, yet it is unknown whether this is a bystander event or a driver of tumorigenesis. We found that overexpression of lysine-specific demethylase 4A (KDM4A, also known as JMJD2A) was positively correlated with Gleason score and metastasis in human prostate tumors. Overexpression of JMJD2A resulted in the development of prostatic intraepithelial neoplasia in mice, demonstrating that JMJD2A can initiate prostate cancer development. Moreover, combined overexpression of JMJD2A and the ETS transcription factor ETV1, a JMJD2A-binding protein, resulted in prostate carcinoma formation in mice haplodeficient for the phosphatase and tensin homolog (Pten) tumor-suppressor gene. Additionally, JMJD2A cooperated with ETV1 to increase expression of yes associated protein 1 (YAP1), a Hippo pathway component that itself was associated with prostate tumor aggressiveness. ETV1 facilitated the recruitment of JMJD2A to the YAP1 promoter, leading to changes in histone lysine methylation in a human prostate cancer cell line. Further, YAP1 expression largely rescued the growth inhibitory effects of JMJD2A depletion in prostate cancer cells, indicating that YAP1 is a downstream effector of JMJD2A. Taken together, these data reveal a JMJD2A/ETV1/YAP1 axis that promotes prostate cancer initiation and that may be a suitable target for therapeutic inhibition. [ABSTRACT FROM AUTHOR]

Published

2016