Search

Your search keyword '"Macinnes, A.W."' showing total 11 results
Start Over Author "Macinnes, A.W."
11 results on '"Macinnes, A.W."'

1. Ribosomal protein gene RPL9 variants can differentially impair ribosome function and cellular metabolism

Author

Lezzerini, M., Penzo, M., O'Donohue, M.F., Vieira, C. Marques Dos San, Saby, M., Elfrink, H.L., Diets, I.J., Hesse, A.M., Coute, Y., Gastou, M., Nin-Velez, A., Nikkels, P.G., Olson, A.N., Zonneveld-Huijssoon, E., Jongmans, M.C.J., Zhang, G., Weeghel, M. van, Houtkooper, R.H., Wlodarski, M.W., Kuiper, R.P, Bierings, M.B., Bosch, J, Leblanc, T., Montanaro, L., Dinman, J.D., Costa, L., Gleizes, P.E., Macinnes, A.W., Lezzerini, M., Penzo, M., O'Donohue, M.F., Vieira, C. Marques Dos San, Saby, M., Elfrink, H.L., Diets, I.J., Hesse, A.M., Coute, Y., Gastou, M., Nin-Velez, A., Nikkels, P.G., Olson, A.N., Zonneveld-Huijssoon, E., Jongmans, M.C.J., Zhang, G., Weeghel, M. van, Houtkooper, R.H., Wlodarski, M.W., Kuiper, R.P, Bierings, M.B., Bosch, J, Leblanc, T., Montanaro, L., Dinman, J.D., Costa, L., Gleizes, P.E., and Macinnes, A.W.

Abstract

Contains fulltext : 218593.pdf (publisher's version ) (Open Access), Variants in ribosomal protein (RP) genes drive Diamond-Blackfan anemia (DBA), a bone marrow failure syndrome that can also predispose individuals to cancer. Inherited and sporadic RP gene variants are also linked to a variety of phenotypes, including malignancy, in individuals with no anemia. Here we report an individual diagnosed with DBA carrying a variant in the 5'UTR of RPL9 (uL6). Additionally, we report two individuals from a family with multiple cancer incidences carrying a RPL9 missense variant. Analysis of cells from these individuals reveals that despite the variants both driving pre-rRNA processing defects and 80S monosome reduction, the downstream effects are remarkably different. Cells carrying the 5'UTR variant stabilize TP53 and impair the growth and differentiation of erythroid cells. In contrast, ribosomes incorporating the missense variant erroneously read through UAG and UGA stop codons of mRNAs. Metabolic profiles of cells carrying the 5'UTR variant reveal an increased metabolism of amino acids and a switch from glycolysis to gluconeogenesis while those of cells carrying the missense variant reveal a depletion of nucleotide pools. These findings indicate that variants in the same RP gene can drive similar ribosome biogenesis defects yet still have markedly different downstream consequences and clinical impacts.

Published
2020

2. Zebrafish Models of Cancer

Author

MacInnes, A.W., Amsterdam, A., Hopkins, N., Lees, J., and Hubrecht Instituut voor Ontwikkelingsbiologie en Stamcelonderzoek

Published
2012

3. Extensive localization of long noncoding RNAs to the cytosol and mono- and polyribosomal complexes

Author

Heesch, S. van, Iterson, M. van, Jacobi, J., Boymans, S., Essers, P.B., Bruijn, E. de, Hao, W., Macinnes, A.W., Cuppen, E., Simonis, M., Heesch, S. van, Iterson, M. van, Jacobi, J., Boymans, S., Essers, P.B., Bruijn, E. de, Hao, W., Macinnes, A.W., Cuppen, E., and Simonis, M.

Abstract

Contains fulltext : 138006.pdf (publisher's version ) (Open Access), BACKGROUND: Long noncoding RNAs (lncRNAs) form an abundant class of transcripts, but the function of the majority of them remains elusive. While it has been shown that some lncRNAs are bound by ribosomes, it has also been convincingly demonstrated that these transcripts do not code for proteins. To obtain a comprehensive understanding of the extent to which lncRNAs bind ribosomes, we performed systematic RNA sequencing on ribosome-associated RNA pools obtained through ribosomal fractionation and compared the RNA content with nuclear and (non-ribosome bound) cytosolic RNA pools. Results : The RNA composition of the subcellular fractions differs significantly from each other, but lncRNAs are found in all locations. A subset of specific lncRNAs is enriched in the nucleus but surprisingly the majority is enriched in the cytosol and in ribosomal fractions. The ribosomal enriched lncRNAs include H19 and TUG1. CONCLUSIONS: Most studies on lncRNAs have focused on the regulatory function of these transcripts in the nucleus. We demonstrate that only a minority of all lncRNAs are nuclear enriched. Our findings suggest that many lncRNAs may have a function in cytoplasmic processes, and in particular in ribosome complexes.

Published
2014

5. Insulin/IGF-1-mediated longevity is marked by reduced protein metabolism

Author

Stout, G.J., Stigter, E.C., Essers, P.B., Mulder, K.W., Kolkman, A., Snijders, D.S., van den Broek, N.J., Betist, M.C., Korswagen, H.C., MacInnes, A.W., Brenkman, A.B., Stout, G.J., Stigter, E.C., Essers, P.B., Mulder, K.W., Kolkman, A., Snijders, D.S., van den Broek, N.J., Betist, M.C., Korswagen, H.C., MacInnes, A.W., and Brenkman, A.B.

Abstract

Mutations in the daf-2 gene of the conserved Insulin/Insulin-like Growth Factor (IGF-1) pathway double the lifespan of the nematode Caenorhabditis elegans. This phenotype is completely suppressed by deletion of Forkhead transcription factor daf-16. To uncover regulatory mechanisms coordinating this extension of life, we employed a quantitative proteomics strategy with daf-2 mutants in comparison with N2 and daf-16; daf-2 double mutants. This revealed a remarkable longevity-specific decrease in proteins involved in mRNA processing and transport, the translational machinery, and protein metabolism. Correspondingly, the daf-2 mutants display lower amounts of mRNA and 20S proteasome activity, despite maintaining total protein levels equal to that observed in wild types. Polyribosome profiling in the daf-2 and daf-16;daf-2 double mutants confirmed a daf-16-dependent reduction in overall translation, a phenotype reminiscent of Dietary Restriction-mediated longevity, which was independent of germline activity. RNA interference (RNAi)-mediated knockdown of proteins identified by our approach resulted in modified C. elegans lifespan confirming the importance of these processes in Insulin/IGF-1-mediated longevity. Together, the results demonstrate a role for the metabolism of proteins in the Insulin/IGF-1-mediated extension of life., Mutations in the daf-2 gene of the conserved Insulin/Insulin-like Growth Factor (IGF-1) pathway double the lifespan of the nematode Caenorhabditis elegans. This phenotype is completely suppressed by deletion of Forkhead transcription factor daf-16. To uncover regulatory mechanisms coordinating this extension of life, we employed a quantitative proteomics strategy with daf-2 mutants in comparison with N2 and daf-16; daf-2 double mutants. This revealed a remarkable longevity-specific decrease in proteins involved in mRNA processing and transport, the translational machinery, and protein metabolism. Correspondingly, the daf-2 mutants display lower amounts of mRNA and 20S proteasome activity, despite maintaining total protein levels equal to that observed in wild types. Polyribosome profiling in the daf-2 and daf-16;daf-2 double mutants confirmed a daf-16-dependent reduction in overall translation, a phenotype reminiscent of Dietary Restriction-mediated longevity, which was independent of germline activity. RNA interference (RNAi)-mediated knockdown of proteins identified by our approach resulted in modified C. elegans lifespan confirming the importance of these processes in Insulin/IGF-1-mediated longevity. Together, the results demonstrate a role for the metabolism of proteins in the Insulin/IGF-1-mediated extension of life.

Published
2013

7. A zebrafish model of dyskeratosis congenita reveals hematopoietic stem cell formation failure resulting from ribosomal protein-mediated p53 stabilization

Author

Pereboom, T.C., van Weele, L.J., Bondt, A., MacInnes, A.W., Pereboom, T.C., van Weele, L.J., Bondt, A., and MacInnes, A.W.

Abstract

Dyskeratosis congenita (DC) is a bone marrow failure disorder characterized by shortened telomeres, defective stem cell maintenance, and highly heterogeneous phenotypes affecting predominantly tissues that require high rates of turnover. Here we present a mutant zebrafish line with decreased expression of nop10, one of the known H/ACA RNP complex genes with mutations linked to DC. We demonstrate that this nop10 loss results in 18S rRNA processing defects and collapse of the small ribosomal subunit, coupled to stabilization of the p53 tumor suppressor protein through small ribosomal proteins binding to Mdm2. These mutants also display a hematopoietic stem cell deficiency that is reversible on loss of p53 function. However, we detect no changes in telomere length in nop10 mutants. Our data support a model of DC whereupon in early development mutations involved in the H/ACA complex contribute to bone marrow failure through p53 deregulation and loss of initial stem cell numbers while their role in telomere maintenance does not contribute to DC until later in life., Dyskeratosis congenita (DC) is a bone marrow failure disorder characterized by shortened telomeres, defective stem cell maintenance, and highly heterogeneous phenotypes affecting predominantly tissues that require high rates of turnover. Here we present a mutant zebrafish line with decreased expression of nop10, one of the known H/ACA RNP complex genes with mutations linked to DC. We demonstrate that this nop10 loss results in 18S rRNA processing defects and collapse of the small ribosomal subunit, coupled to stabilization of the p53 tumor suppressor protein through small ribosomal proteins binding to Mdm2. These mutants also display a hematopoietic stem cell deficiency that is reversible on loss of p53 function. However, we detect no changes in telomere length in nop10 mutants. Our data support a model of DC whereupon in early development mutations involved in the H/ACA complex contribute to bone marrow failure through p53 deregulation and loss of initial stem cell numbers while their role in telomere maintenance does not contribute to DC until later in life.

Published
2011

8. Perinatal exogenous nitric oxide in fawn-hooded hypertensive rats reduces renal ribosomal biogenesis in early life

Author

Wesseling, S., Essers, P.B., Koeners, M.P., Pereboom, T.C., Braam, B., van Faassen, E.E., MacInnes, A.W., Joles, J.A., Wesseling, S., Essers, P.B., Koeners, M.P., Pereboom, T.C., Braam, B., van Faassen, E.E., MacInnes, A.W., and Joles, J.A.

Abstract

Nitric oxide (NO) is known to depress ribosome biogenesis in vitro. In this study we analyzed the influence of exogenous NO on ribosome biogenesis in vivo using a proven antihypertensive model of perinatal NO administration in genetically hypertensive rats. Fawn-hooded hypertensive rat (FHH) dams were supplied with the NO-donor molsidomine in drinking water from 2 weeks before to 4 weeks after birth, and the kidneys were subsequently collected from 2 day, 2 week, and 9 to 10-month-old adult offspring. Although the NO-donor increased maternal NO metabolite excretion, the NO status of juvenile renal (and liver) tissue was unchanged as assayed by EPR spectroscopy of NO trapped with iron-dithiocarbamate complexes. Nevertheless, microarray analysis revealed marked differential up-regulation of renal ribosomal protein genes at 2 days and down-regulation at 2 weeks and in adult males. Such differential regulation of renal ribosomal protein genes was not observed in females. These changes were confirmed in males at 2 weeks by expression analysis of renal ribosomal protein L36a and by polysome profiling, which also revealed a down-regulation of ribosomes in females at that age. However, renal polysome profiles returned to normal in adults after early exposure to molsidomine. No direct effects of molsidomine were observed on cellular proliferation in kidneys at any age, and the changes induced by molsidomine in renal polysome profiles at 2 weeks were absent in the livers of the same rats. Our results suggest that the previously found prolonged antihypertensive effects of perinatal NO administration may be due to epigenetically programmed alterations in renal ribosome biogenesis during a critical fetal period of renal development, and provide a salient example of a drug-induced reduction of ribosome biogenesis that is accompanied by a beneficial long-term health effect in both males and females. Keywords: nitric oxide, ribosomal biogenesis, microarray, polysome profiling, peri, Nitric oxide (NO) is known to depress ribosome biogenesis in vitro. In this study we analyzed the influence of exogenous NO on ribosome biogenesis in vivo using a proven antihypertensive model of perinatal NO administration in genetically hypertensive rats. Fawn-hooded hypertensive rat (FHH) dams were supplied with the NO-donor molsidomine in drinking water from 2 weeks before to 4 weeks after birth, and the kidneys were subsequently collected from 2 day, 2 week, and 9 to 10-month-old adult offspring. Although the NO-donor increased maternal NO metabolite excretion, the NO status of juvenile renal (and liver) tissue was unchanged as assayed by EPR spectroscopy of NO trapped with iron-dithiocarbamate complexes. Nevertheless, microarray analysis revealed marked differential up-regulation of renal ribosomal protein genes at 2 days and down-regulation at 2 weeks and in adult males. Such differential regulation of renal ribosomal protein genes was not observed in females. These changes were confirmed in males at 2 weeks by expression analysis of renal ribosomal protein L36a and by polysome profiling, which also revealed a down-regulation of ribosomes in females at that age. However, renal polysome profiles returned to normal in adults after early exposure to molsidomine. No direct effects of molsidomine were observed on cellular proliferation in kidneys at any age, and the changes induced by molsidomine in renal polysome profiles at 2 weeks were absent in the livers of the same rats. Our results suggest that the previously found prolonged antihypertensive effects of perinatal NO administration may be due to epigenetically programmed alterations in renal ribosome biogenesis during a critical fetal period of renal development, and provide a salient example of a drug-induced reduction of ribosome biogenesis that is accompanied by a beneficial long-term health effect in both males and females. Keywords: nitric oxide, ribosomal biogenesis, microarray, polysome profiling, peri

Published
2011

9. The nucleolar GTP-binding proteins Gnl2 and nucleostemin are required for retinal neurogenesis in developing zebrafish

Author

Paridaen, J.T.M., Janson, E., Utami, K.H., Pereboom, T.C., Essers, P., van Rooijen, C.R., Zivkovic, D., MacInnes, A.W., Paridaen, J.T.M., Janson, E., Utami, K.H., Pereboom, T.C., Essers, P., van Rooijen, C.R., Zivkovic, D., and MacInnes, A.W.

Abstract

Nucleostemin (NS), a member of a family of nucleolar GTP-binding proteins, is highly expressed in proliferating cells such as stem and cancer cells and is involved in the control of cell cycle progression. Both depletion and overexpression of NS result in stabilization of the tumor suppressor p53 protein in vitro. Although it has been previously suggested that NS has p53-independent functions, these to date remain unknown. Here, we report two zebrafish mutants recovered from forward and reverse genetic screens that carry loss of function mutations in two members of this nucleolar protein family, Guanine nucleotide binding-protein-like 2 (Gnl2) and Gnl3/NS. We demonstrate that these proteins are required for correct timing of cell cycle exit and subsequent neural differentiation in the brain and retina. Concomitantly, we observe aberrant expression of the cell cycle regulators cyclinD1 and p57kip2. Our models demonstrate that the loss of Gnl2 or NS induces p53 stabilization and p53-mediated apoptosis. However, the retinal differentiation defects are independent of p53 activation. Furthermore, this work demonstrates that Gnl2 and NS have both non-cell autonomously and cell-autonomous function in correct timing of cell cycle exit and neural differentiation. Finally, the data suggest that Gnl2 and NS affect cell cycle exit of neural progenitors by regulating the expression of cell cycle regulators independently of p53. [KEYWORDS: Animals, Blotting, Western, Bromodeoxyuridine, Cell Cycle/ physiology, Cyclin D1/metabolism, Cyclin-Dependent Kinase Inhibitor p57/metabolism, GTP-Binding Proteins/genetics/ metabolism, Gene Expression Regulation/ physiology, Immunohistochemistry, In Situ Hybridization, Microarray Analysis, Microscopy, Fluorescence, Mutation/genetics, Neurogenesis/ physiology, Nuclear Proteins/genetics/ metabolism, Oligonucleotides/genetics, Plasmids/genetics, Retina/ embryology, Zebrafish/ embryology, Nucleostemin (NS), a member of a family of nucleolar GTP-binding proteins, is highly expressed in proliferating cells such as stem and cancer cells and is involved in the control of cell cycle progression. Both depletion and overexpression of NS result in stabilization of the tumor suppressor p53 protein in vitro. Although it has been previously suggested that NS has p53-independent functions, these to date remain unknown. Here, we report two zebrafish mutants recovered from forward and reverse genetic screens that carry loss of function mutations in two members of this nucleolar protein family, Guanine nucleotide binding-protein-like 2 (Gnl2) and Gnl3/NS. We demonstrate that these proteins are required for correct timing of cell cycle exit and subsequent neural differentiation in the brain and retina. Concomitantly, we observe aberrant expression of the cell cycle regulators cyclinD1 and p57kip2. Our models demonstrate that the loss of Gnl2 or NS induces p53 stabilization and p53-mediated apoptosis. However, the retinal differentiation defects are independent of p53 activation. Furthermore, this work demonstrates that Gnl2 and NS have both non-cell autonomously and cell-autonomous function in correct timing of cell cycle exit and neural differentiation. Finally, the data suggest that Gnl2 and NS affect cell cycle exit of neural progenitors by regulating the expression of cell cycle regulators independently of p53. [KEYWORDS: Animals, Blotting, Western, Bromodeoxyuridine, Cell Cycle/ physiology, Cyclin D1/metabolism, Cyclin-Dependent Kinase Inhibitor p57/metabolism, GTP-Binding Proteins/genetics/ metabolism, Gene Expression Regulation/ physiology, Immunohistochemistry, In Situ Hybridization, Microarray Analysis, Microscopy, Fluorescence, Mutation/genetics, Neurogenesis/ physiology, Nuclear Proteins/genetics/ metabolism, Oligonucleotides/genetics, Plasmids/genetics, Retina/ embryology, Zebrafish/ embryology

Published
2011

10. 'Mitochondrial communication is key': Cross-compartmental signals maintaining proteostasis and longevity

Author

Molenaars, M., Houtkooper, Riekelt H. L., Janssens, Georges E., Maccines, A. W., Laboratory Genetic Metabolic Diseases, Amsterdam Gastroenterology Endocrinology Metabolism, Graduate School, Houtkooper, R.H., Janssens, G., MacInnes, A.W., and Faculteit der Geneeskunde

Abstract

Aging is a complex biological phenomenon. Better understanding of underlying mechanisms of aging promotes development of preventative therapies for chronic, degenerative age-related diseases such as type 2 diabetes, obesity, cardiovascular disease, cancer and Alzheimer's disease. While aging has long been considered a passive process, evidence has accumulated in model organisms that targeting specific cellular pathways strongly affects health and longevity. This thesis presents insights into the cellular processes related to aging, with an underlying quest for understanding how cellular cross-compartmental signals ensure longevity. Mitochondria are the compartments responsible for producing energy in the cell. While mitochondria produce energy, one of the processes in the cell that consumes most energy is translation of mRNA into protein carried out by ribosomes. In this thesis we show how mitochondrial communication and metabolism can regulate the aging process. For instance by slowing down protein synthesis. Using less energy by slowing down mitochondria, and simultaneously synthesizing less new proteins by having less ribosomes, leads to a more sustainable state of the cell overall. To maintain sustainability, signals are sent, inducing processes such as proteostasis and quality control to ultimately lead to cytoprotection and longevity. The more we know on the precise mechanisms of mitochondrial compartmental signaling, the more we could exploit these for possible treatments. With the human population getting older, and the last years of life often being accompanied by age-related diseases, therapeutic approaches that could prevent these diseases would have a huge impact.

Published
2020

11. In Profile: Models of Ribosome Biogenesis Defects and Regulation of Protein Synthesis

Author

Essers, P.B.M., Cuppen, Edwin, MacInnes, A.W., and University Utrecht

Subjects
Econometric and Statistical Methods: General, Geneeskunde (GENK), Bescherming en bevordering van de menselijke gezondheid, Geneeskunde(GENK), Medical sciences, General [Econometric and Statistical Methods]
Abstract

Ribosomes are the mediators of protein synthesis in the cell and therefore crucial to proper cell function. In addition, ribosomes are highly abundant, with ribosomal RNA making up 80% of the RNA in the cell. A large amount of resources go into maintaining this pool of ribosomes, so ribosome biogenesis and translation are highly controlled mechanisms. In this thesis we explore both ribosome biogenesis defects and physiological control of ribosome numbers and translation efficiency. In the first part of this thesis, we examined the role the nucleostemin gene family plays in ribosome biogenesis. We provide evidence that gnl2 and nucleostemin (ns), but not gnl3l, are required for ribosome biogenesis. All three mutants stabilize p53, which in ns is believed to occur through ribosomal stress, but in gnl3l occurs through another, as of yet unidentified mechanism. We argue that the overexpression of neural progenitor genes that we observe in the gnl2 and ns mutants is most likely a secondary effect of their ribosome biogenesis defects, since other ribosome biogenesis mutants display similar phenotypes. Inactivation of the insulin/insulin growth factor signalling (IIS) pathway in C elegans results in a remarkable increase in lifespan. In the second part of this thesis, we identified a strong downregulation of protein metabolism in a IIS mutant that was previously overlooked, using an unbiased mass spectrometry approach. This links the pathways of insulin/insulin growth factor signalling and dietary restriction mediated longevity more closely than was previously appreciated. In addition to a reduction in global translation, we also observed altered translation efficiency for several subsets of mRNAs. We identified a number of ribosome associated ncRNAs and provided evidence that one of these, tts-1, inhibits polysome formation and extends lifespan. In the last part of this thesis, unrelated to ribosomes, we investigated the interaction between the Von Hippel-Lindau (VHL) and the p53 tumour suppressors in a zebrafish model of vhl loss. In contrast to earlier in vitro studies, we observed increased stabilization of p53 in the absence of vhl. We identified a novel interaction between VHL and PDCD5 and showed that loss of VHL results in nuclear translocation of PDCD5 and subsequent degradation of MDM2, leading to increased p53 stabilization and target gene transcription. However, vhl is required for caspase activation and apoptosis to occur in response to DNA damage. These findings possibly explain why VHL and p53 are rarely found both mutated in RCC, since loss of p53 would not confer any additional growth advantage to VHL negative cells.

Published
2013

Catalog

Books, media, physical & digital resources
See catalog results