Your search keyword '"Duplomb, Laurence"' showing total 26 results

1. Serpin B1 defect and increased apoptosis of neutrophils in Cohen syndrome neutropenia.

Author

Duplomb, Laurence, Rivière, Julie, Jego, Gaëtan, Da Costa, Romain, Hammann, Arlette, Racine, Jessica, Schmitt, Alain, Droin, Nathalie, Capron, Claude, Gougerot-Pocidalo, Marie-Anne, Dubrez, Laurence, Aral, Bernard, Lafon, Arnaud, Edery, Patrick, Ghoumid, Jamal, Blair, Edward, El Chehadeh-Djebbar, Salima, Carmignac, Virginie, Thevenon, Julien, and Guy, Julien

Subjects

*NEUTROPHILS, *LEUCOCYTE elastase, *GOLGI apparatus, *CELL death, *APOPTOSIS, *GENETIC disorders

Abstract

Cohen syndrome (CS) is a rare genetic disorder due to mutations in VPS13B gene. Among various clinical and biological features, CS patients suffer from inconsistent neutropenia, which is associated with recurrent but minor infections. We demonstrate here that this neutropenia results from an exaggerate rate of neutrophil apoptosis. Besides this increased cell death, which occurs in the absence of any endoplasmic reticulum stress or defect in neutrophil elastase (ELANE) expression or localization, all neutrophil functions appeared to be normal. We showed a disorganization of the Golgi apparatus in CS neutrophils precursors, that correlates with an altered glycosylation of ICAM-1 in these cells, as evidenced by a migration shift of the protein. Furthermore, a striking decrease in the expression of SERPINB1 gene, which encodes a critical component of neutrophil survival, was detected in CS neutrophils. These abnormalities may account for the excessive apoptosis of neutrophils leading to neutropenia in CS. Key messages: Cohen syndrome patients' neutrophils display normal morphology and functions. Cohen syndrome patients' neutrophils have an increased rate of spontaneous apoptosis compared to healthy donors' neutrophils. No ER stress or defective ELA2 expression or glycosylation was observed in Cohen syndrome patients' neutrophils. SerpinB1 expression is significantly decreased in Cohen syndrome neutrophils as well as in VPS13B-deficient cells. [ABSTRACT FROM AUTHOR]

Published

2019

2. A first-in-class inhibitor of HSP110 to potentiate XPO1-targeted therapy in primary mediastinal B-cell lymphoma and classical Hodgkin lymphoma.

Author

Durand, Manon, Cabaud Gibouin, Vincent, Duplomb, Laurence, Salmi, Leila, Caillot, Mélody, Sola, Brigitte, Camus, Vincent, Jardin, Fabrice, Garrido, Carmen, and Jego, Gaëtan

Subjects

*HODGKIN'S disease, *HEMATOLOGIC malignancies, *STAT proteins, *CELLULAR signal transduction, *CELL size, *TALL-1 (Protein)

Abstract

Background: Primary mediastinal B-cell lymphoma (PMBL) and classical Hodgkin lymphoma (cHL) are distinct hematological malignancies of B-cell origin that share many biological, molecular, and clinical characteristics. In particular, the JAK/STAT signaling pathway is a driver of tumor development due to multiple recurrent mutations, particularly in STAT6. Furthermore, the XPO1 gene that encodes exportin 1 (XPO1) shows a frequent point mutation (E571K) resulting in an altered export of hundreds of cargo proteins, which may impact the success of future therapies in PMBL and cHL. Therefore, targeted therapies have been envisioned for these signaling pathways and mutations. Methods: To identify novel molecular targets that could overcome the treatment resistance that occurs in PMBL and cHL patients, we have explored the efficacy of a first-in-class HSP110 inhibitor (iHSP110-33) alone and in combination with selinexor, a XPO1 specific inhibitor, both in vitro and in vivo. Results: We show that iHSP110-33 decreased the survival of several PMBL and cHL cell lines and the size of tumor xenografts. We demonstrate that HSP110 is a cargo of XPO1wt as well as of XPO1E571K. Using immunoprecipitation, proximity ligation, thermophoresis and kinase assays, we showed that HSP110 directly interacts with STAT6 and favors its phosphorylation. The combination of iHSP110-33 and selinexor induces a synergistic reduction of STAT6 phosphorylation and of lymphoma cell growth in vitro and in vivo. In biopsies from PMBL patients, we show a correlation between HSP110 and STAT6 phosphorylation levels. Conclusions: These findings suggest that HSP110 could be proposed as a novel target in PMBL and cHL therapy. [ABSTRACT FROM AUTHOR]

Published

2024

3. Osteoprotegerin: Multiple partners for multiple functions.

Author

Baud’huin, Marc, Duplomb, Laurence, Teletchea, Stéphane, Lamoureux, François, Ruiz-Velasco, Carmen, Maillasson, Mike, Redini, Françoise, Heymann, Marie-Françoise, and Heymann, Dominique

Subjects

*OSTEOPROTEGERIN, *OSTEONECTIN, *TRANCE protein, *OSTEOCLASTS, *CELL differentiation, *TUMOR necrosis factors

Abstract

Abstract: Osteoprotegerin (OPG) is an essential secreted protein in bone turnover due to its role as a decoy receptor for the Receptor Activator of Nuclear Factor-kB ligand (RANKL) in the osteoclasts, thus inhibiting their differentiation. However, there are additional ligands of OPG that confer various biological functions. OPG can promote cell survival, cell proliferation and facilitates migration by binding TNF-related apoptosis inducing ligand (TRAIL), glycosaminoglycans or proteoglycans. A large number of in vitro, pre-clinical and clinical studies provide evidences of OPG involvement in vascular, bone, immune and tumor biology. This review describes an overview of the different OPG ligands regulating its biological functions. [Copyright &y& Elsevier]

Published

2013

4. The dual role of IL-6-type cytokines on bone remodeling and bone tumors

Author

Blanchard, Frédéric, Duplomb, Laurence, Baud’huin, Marc, and Brounais, Bénédicte

Subjects

*BONE remodeling, *BONE tumors, *INTERLEUKIN-6, *CYTOKINES, *BONE cells, *PROTEIN kinases

Abstract

Abstract: Many factors such as vitamins, hormones and cytokines, control bone metabolism and remodeling. Cytokines of the interleukin-6 family, by acting on bone cells (i.e. osteoblasts and osteoclasts), have an important role in the bone tissue but they recently appeared as double-edged swords. They sustain bone formation but they can also drive bone loss in various osteolytic pathologies. Similarly, development of bone cancers can be either prevented or enhanced by these cytokines, depending on the cell type, the stage of the tumor and the bone environment. This dual effect is also apparent at the level of the signal transducer and activator of transcription and the mitogen-activated protein kinases, the two main signaling pathways that mediate opposite effects in bone cells. [Copyright &y& Elsevier]

Published

2009

5. Hepatic insig-1 or -2 overexpression reduces lipogenesis in obese Zucker diabetic fatty rats and in fasted/refed normal rats.

Author

Takaishi, Kiyosumi, Duplomb, Laurence, May-Yn Wang, Jinping Li, and Unger, Roger H.

Subjects

*GENE expression, *LABORATORY rats, *LIVER, *DIABETES, *ADENOVIRUSES, *FATTY degeneration

Abstract

To determine whether the antilipogenic actions of insulin-induced gene 1 (insig-1) demonstrated in cultured preadipocytes also occur in vivo, we infected Zucker diabetic fatty (ZDF) (fa/fa) rats, with recombinant adenovirus containing insig-1 or -2 cDNA. An increase of both proteins appeared in their livers. In control ZDF (fa/fa) rats infected with adenovirus containing the β-galactosidase (β-gal) cDNA, triacylglycerols in the liver and plasma rose steeply whereas the insig-infected rats exhibited substantial attenuation of the increase in hepatic steatosis and hyperlipidemia. Insig overexpression was associated with a striking reduction in the elevated level of nuclear sterol regulatory element-binding protein (SREBP)-1c, the activated form of the transcription factor. The mRNA of SREBP-1c lipogenic target enzymes also fell. The mRNA of endogenous insig-1, but not -2a and -2b, was higher in the fatty livers of untreated obese ZDF (fa/fa) rats compared with controls, but the elevation was not sufficient to block the ≈3-fold increase in SREBP-1c expression and activity. In normal animals, adenovirus-induced overexpression of the insigs reduced the increase in SREBP-1c mRNA and its target enzymes caused by refeeding. The findings demonstrated that both insigs have antilipogenic action when transgenically overexpressed in livers with increased SREBP-1c-mediated lipogenesis. However, the increase in endogenous insig-1 expression associated with augmented lipogenesis may limit it, but is insufficient to prevent it. [ABSTRACT FROM AUTHOR]

Published

2004

6. Increased expression and activity of 11β-HSD-1 in diabetic islets and prevention with troglitazone

Author

Duplomb, Laurence, Lee, Young, Wang, May-Yun, Park, Byung H., Takaishi, Kiyosumi, Agarwal, Anil K., and Unger, Roger H.

Subjects

*GLUCOCORTICOIDS, *PANCREATIC diseases, *CUSHING'S syndrome, *OBESITY

Abstract

To determine if increased local production of glucocorticoids by the pancreatic islets might play a role in the spontaneous noninsulin-dependent diabetes mellitus of obesity, we compared islet 11β-HSD-1 mRNA and activity in islets of obese prediabetic and diabetic Zucker Diabetic Fatty (ZDF) (fa/fa) rats and lean wild-type (+/+) controls. In diabetic rat islets, both mRNA and enzymatic activity of the enzyme were increased in proportion to the hyperglycemia. Troglitazone (TGZ) treatment, beginning at 6 weeks of age, prevented the hyperglycemia, the hyperlipidemia, and the increase in 11β-HSD-1. To determine if the metabolic abnormalities had caused the 11β-HSD-1 increase, prediabetic islets were cultured in high or low glucose or in 2:1 oleate:palmitate for 3 days. Neither nutrient enhanced the expression of 11β-HSD-1. We conclude that 11β-HSD-1 expression and activity are increased in islets of diabetic, but not prediabetic ZDF rats, and that TGZ prevents both the increase in 11β-HSD-1 and the diabetes. [Copyright &y& Elsevier]

Published

2004

7. Independence of hyperleptinemia-induced fat disappearance from thyroid hormone

Author

Duplomb, Laurence, Takaishi, Kiyosumi, Park, Byung-Hyun, Visser, Theo J., and Unger, Roger H.

Subjects

*THYROID hormones, *HYPERTHYROIDISM, *CARBOXYLIC acids, *RATS

Abstract

Sustained hyperleptinemia induced in normal rats causes the rapid disappearance of body fat. This is attributed to a marked increase in uncoupled fatty acid oxidation in the white adipocytes, which also occurs in hyperthyroidism. Because hyperleptinemic rats have normal plasma T3 or T4 levels, we tested the possibility of “localized hyperthyroidism” due to increased conversion of T4 to T3 in the adipose tissue. We therefore induced sustained hyperleptinemia in normal rats by intravenous injection of recombinant adenovirus containing the leptin cDNA (AdCMV-leptin) and measured the mRNA and the activity of enzymes involved in T4 metabolism in the disappearing fat. The epididymal fat pad remnants exhibited a decrease in mRNA of deiodinase 1 and a doubling of deiodinase 2 mRNA (p<0.05), but their enzyme activities did not differ from normoleptinemic controls. To determine if thyroid hormone was required for the fat-wasting action of hyperleptinemia, we infused AdCMV-leptin into rats made athyroid by total thyroidectomy or by methimazole therapy. The fat loss in hyperleptinemic athyroid rats was as great as in euthyroid controls. We conclude that the fat-wasting effect of sustained hyperleptinemia does not involve “local hyperthyroidism” in white adipose tissue and does not require thyroid hormone. [Copyright &y& Elsevier]

Published

2004

8. IL-6 inhibits RANKL-induced osteoclastogenesis by diverting cells into the macrophage lineage: Key role of serine727 phosphorylation of STAT3

Author

Duplomb, Laurence, Baud'Huin, Marc, Charrier, Celine, Trichet, Valerie, Blanchard, Frederic, and Heymann, Dominique

Published

2008

9. Autosomal-recessive SASH1 variants associated with a new genodermatosis with pigmentation defects, palmoplantar keratoderma and skin carcinoma.

Author

Courcet, Jean- Benoît, Elalaoui, Siham Chafai, Duplomb, Laurence, Tajir, Mariam, Rivière, Jean-Baptiste, Thevenon, Julien, Gigot, Nadège, Marle, Nathalie, Aral, Bernard, Duffourd, Yannis, Sarasin, Alain, Naim, Valeria, Courcet-Degrolard, Emilie, Aubriot-Lorton, Marie- Hélène, Martin, Laurent, Abrid, Jamal Eddin, Thauvin, Christel, Sefiani, Abdelaziz, Vabres, Pierre, and Faivre, Laurence

Subjects

*HUMAN skin color genetics, *SKIN cancer, *PALMOPLANTAR keratoderma, *TUMOR suppressor genes, *NEOPLASTIC cell transformation

Abstract

SASH1 (SAM and SH3 domain-containing protein 1) is a tumor suppressor gene involved in the tumorigenesis of a spectrum of solid cancers. Heterozygous SASH1 variants are known to cause autosomal-dominant dyschromatosis. Homozygosity mapping and whole-exome sequencing were performed in a consanguineous Moroccan family with two affected siblings presenting an unclassified phenotype associating an abnormal pigmentation pattern (hypo- and hyperpigmented macules of the trunk and face and areas of reticular hypo- and hyperpigmentation of the extremities), alopecia, palmoplantar keratoderma, ungueal dystrophy and recurrent spinocellular carcinoma. We identified a homozygous variant in SASH1 (c.1849G>A; p.Glu617Lys) in both affected individuals. Wound-healing assay showed that the patient's fibroblasts were better able than control fibroblasts to migrate. Following the identification of SASH1 heterozygous variants in dyschromatosis, we used reverse phenotyping to show that autosomal-recessive variants of this gene could be responsible for an overlapping but more complex phenotype that affected skin appendages. SASH1 should be added to the list of genes responsible for autosomal-dominant and -recessive genodermatosis, with no phenotype in heterozygous patients in the recessive form, and to the list of genes responsible for a predisposition to skin cancer. [ABSTRACT FROM AUTHOR]

Published

2015

10. PIK3R1 Mutations Cause Syndromic Insulin Resistance with Lipoatrophy.

Author

Thauvin-Robinet, Christel, Auclair, Martine, Duplomb, Laurence, Caron-Debarle, Martine, Avila, Magali, St-Onge, Judith, Le?Merrer, Martine, Le?Luyer, Bernard, Héron, Delphine, Mathieu-Dramard, Michèle, Bitoun, Pierre, Petit, Jean-Michel, Odent, Sylvie, Amiel, Jeanne, Picot, Damien, Carmignac, Virginie, Thevenon, Julien, Callier, Patrick, Laville, Martine, and Reznik, Yves

Subjects

*PHOSPHATIDYLINOSITOL 3-kinases, *GENETIC mutation, *INSULIN resistance, *ATROPHY, *JOINT hypermobility, *INGUINAL hernia

Abstract

Short stature, hyperextensibility of joints and/or inguinal hernia, ocular depression, Rieger anomaly, and teething delay (SHORT) syndrome is a developmental disorder with an unknown genetic cause and hallmarks that include insulin resistance and lack of subcutaneous fat. We ascertained two unrelated individuals with SHORT syndrome, hypothesized that the observed phenotype was most likely due to de novo mutations in the same gene, and performed whole-exome sequencing in the two probands and their unaffected parents. We then confirmed our initial observations in four other subjects with SHORT syndrome from three families, as well as 14 unrelated subjects presenting with syndromic insulin resistance and/or generalized lipoatrophy associated with dysmorphic features and growth retardation. Overall, we identified in nine affected individuals from eight families de novo or inherited PIK3R1 mutations, including a mutational hotspot (c.1945C>T [p.Arg649Trp]) present in four families. PIK3R1 encodes the p85α, p55α, and p50α regulatory subunits of class IA phosphatidylinositol 3 kinases (PI3Ks), which are known to play a key role in insulin signaling. Functional data from fibroblasts derived from individuals with PIK3R1 mutations showed severe insulin resistance for both proximal and distal PI3K-dependent signaling. Our findings extend the genetic causes of severe insulin-resistance syndromes and provide important information with respect to the function of PIK3R1 in normal development and its role in human diseases, including growth delay, Rieger anomaly and other ocular affections, insulin resistance, diabetes, paucity of fat, and ovarian cysts. [Copyright &y& Elsevier]

Published

2013

11. Proteoglycans: key partners in bone cell biology.

Author

Lamoureux, François, Baud'huin, Marc, Duplomb, Laurence, Heymann, Dominique, and Rédini, Fran&#x00E7'oise

Subjects

*PROTEOGLYCANS, *TISSUES, *GLYCOPROTEINS, *BONE resorption, *OSTEOCLASTS, *BONE tumors, *METABOLISM, *TUMOR treatment

Abstract

The article focuses on the different aspects within proteoglycan (PG) metabolism in skeletal tissues. It describes the complex composition of PGs in bone tissues and talks about the role of PGs in mediating osteoclastic activity in physiological and pathological conditions, particularly in bone tumor-associated osteolysis. The therapeutic interest of PGs in bone tumors is also discussed.

Published

2007

12. Hyperleptinemia prevents lipotoxic cardiomyopathy in acyl CoA synthase transgenic mice.

Author

Young Lee, Naseem, R. Haris, Duplomb, Laurence, Byung-Hyun Park, Garry, Daniel J., Richardson, James A., Schaffer, Jean E., and Unger, Roger H.

Subjects

*NUTRITION, *CARDIOMYOPATHIES, *TRANSGENIC animals, *TRANSGENIC mice, *NUTRITION disorders, *ELECTRON microscopes, *FATTY acids, *PRESERVATION of organs, tissues, etc.

Abstract

The physiologic function of the progressive hyperleptinemia of diet-induced obesity is unknown. However, that lipotoxicity in nonadipose tissues of congenitally unleptinized obese rodents is far greater than in hyperleptinemic diet-induced obesity rodents has suggested an antilipotoxic role. To test this hypothesis, mice with severe lipotoxic cardiomyopathy, induced transgenically by cardiomyocyte-specific overexpression of the acyl CoA synthase (ACS) gene, were made hyperleptinemic by treatment with recombinant adenovirus containing the leptin cDNA. Normoleptinemic control ACS-transgenic mice developed severe dilated cardiomyopathy with thickened left ventricular walls and profound impairment of systolic function on echocardiogram; histologically, there was severe myofiber disorganization and interstitial fibrosis, with intracytoplasmic lipid vacuoles identifiable by electron microscope. By contrast, the hearts of hyperleptinemic ACS-transgenic mice appeared normal, with normal echocardiograms and cardiac triglyceride (TG) contents. Their lower myocardial TG content was ascribed primarily to profound lowering of plasma TG and free fatty acids; free fatty acids were 17% of normal at 8 weeks. Additionally, enhanced myocardial AMP-activated protein kinase phosphorylation may have increased fatty acid oxidation, thereby contributing to the lowering of lipid stores. We conclude that obesity-level hyperleptinemia protects the heart from lipotoxicity. [ABSTRACT FROM AUTHOR]

Published

2004

13. Mutations in the Immunoglobulin-like Domain of gp190, the Leukemia Inhibitory Factor (LIF) Receptor, Increase or Decrease Its Affinity for LIF.

Author

Bitard, Juliette, Daburon, Sophie, Duplomb, Laurence, Blanchard, Frédéric, Vuisio, Patricia, Jacques, Yannick, Godard, Anne, Heath, John K., Moreau, Jean-François, and Taupin, Jean-Luc

Subjects

*IMMUNOGLOBULIN G, *LEUKEMIA inhibitory factor, *AMINO acids, *CELL proliferation

Abstract

Demonstrates the role of the immunoglobulin G-like domain in leukemia inhibitory factor (LIF) binding. Potential to modulate receptor affinity in the family with very limited amino acid changes; Production and expression of shgp190myc and its single point mutant; Enhancement of the blocking activity of shgp90 on hLIF-dependent cell proliferation.

Published

2003

14. Cystoid maculopathy is a frequent feature of Cohen syndrome-associated retinopathy.

Author

Gabrielle, Pierre-Henry, Faivre, Laurence, Audo, Isabelle, Zanlonghi, Xavier, Dollfus, Hélène, Thiadens, Alberta A. H. J., Zeitz, Christina, Mancini, Grazia M. S., Perdomo, Yaumara, Mohand-Saïd, Saddek, Lizé, Eléonore, Lhussiez, Vincent, Nandrot, Emeline F., Acar, Niyazi, Creuzot-Garcher, Catherine, Sahel, José-Alain, Ansar, Muhammad, Thauvin-Robinet, Christel, Duplomb, Laurence, and Da Costa, Romain

Subjects

*DYSTROPHY, *OPTICAL coherence tomography, *CARBONIC anhydrase inhibitors, *PHOTORECEPTORS, *CARBONIC anhydrase

Abstract

Cohen syndrome (CS) is a rare syndromic form of rod-cone dystrophy. Recent case reports have suggested that cystoid maculopathy (CM) could affect CS patients with an early onset and high prevalence. Our study aims at improving our understanding and management of CM in CS patients through a retrospective case series of ten CS patients with identified pathogenic variants in VPS13B. Longitudinal optical coherence tomography (OCT) imaging was performed and treatment with carbonic anhydrase inhibitors (CAI) was provided to reduce the volume of cystoid spaces. CM affected eight out of ten patients in our cohort. The youngest patient showed a strong progression of macular cysts from the age of 4.5 to 5 years despite oral CAI medication. Other teenage and young adult patients showed stable macular cysts with and without treatment. One patient showed a moderate decrease of cystoid spaces in the absence of treatment at 22 years of age. Through a correlative analysis we found that the volume of cystoid spaces was positively correlated to the thickness of peripheral and macular photoreceptor-related layers. This study suggests that CAI treatments may not suffice to improve CM in CS patients, and that CM may resolve spontaneously during adulthood as photoreceptor dystrophy progresses. [ABSTRACT FROM AUTHOR]

Published

2021

15. Neutralization of HSF1 in cells from PIK3CA-related overgrowth spectrum patients blocks abnormal proliferation.

Author

Da Costa, Romain, De Almeida, Steven, Chevarin, Martin, Hadj-Rabia, Smail, Leclerc-Mercier, Stéphanie, Thauvin-Robinet, Christel, Garrido, Carmen, Faivre, Laurence, Vabres, Pierre, Duplomb, Laurence, and Jego, Gaëtan

Subjects

*HEAT shock factors, *GENETIC mutation, *CANCER cells, *TRANSCRIPTION factors

Abstract

PIK3CA -related overgrowth spectrum is caused by mosaicism mutations in the PIK3CA gene. These mutations, which are also observed in various types of cancer, lead to a constitutive activation of the PI3K/AKT/mTOR pathway, increasing cell proliferation. Heat shock transcription factor 1 (HSF1) is the major stress-responsive transcription factor. Recent findings indicate that AKT phosphorylates and activates HSF1 independently of heat-shock in breast cancer cells. Here, we aimed to investigate the role of HSF1 in PIK3CA -related overgrowth spectrum. We observed a higher rate of proliferation and increased phosphorylation of AKT and p70S6K in mutant fibroblasts than in control cells. We also found elevated phosphorylation and activation of HSF1, which is directly correlated to AKT activation. Specific AKT inhibitors inhibit HSF1 phosphorylation as well as HSF1-dependent gene transcription. Finally, we demonstrated that targeting HSF1 with specific inhibitors reduced the proliferation of mutant cells. As there is currently no curative treatment for PIK3CA -related overgrowth spectrum, our results identify HSF1 as a new potential therapeutic target. • PIK3CA -related overgrowth spectrum is characterized by increased cell proliferation. • Strong activation of HSF1 is found in PIK3CA -related overgrowth spectrum fibroblasts. • AKT inhibitors reduces HSF1 activation and HSF1-dependent gene transcription. • HSF1 inhibition blocks the PIK3CA -related overgrowth spectrum proliferation. [ABSTRACT FROM AUTHOR]

Published

2020

16. Report of the first patient with a homozygous OTUD7A variant responsible for epileptic encephalopathy and related proteasome dysfunction.

Author

Garret, Philippine, Ebstein, Frédéric, Delplancq, Geoffroy, Dozieres‐Puyravel, Blandine, Boughalem, Aïcha, Auvin, Stéphane, Duffourd, Yannis, Klafack, Sandro, Zieba, Barbara A., Mahmoudi, Sana, Singh, Karun K., Duplomb, Laurence, Thauvin‐Robinet, Christel, Costa, Jean‐Marc, Krüger, Elke, Trost, Detlef, Verloes, Alain, Faivre, Laurence, and Vitobello, Antonio

Subjects

*PROTEASOMES, *FACIAL abnormalities, *CATALYTIC domains, *LEARNING disabilities, *DEVELOPMENTAL delay, *OVARIAN cancer

Abstract

Heterozygous microdeletions of chromosome 15q13.3 (MIM: 612001) show incomplete penetrance and are associated with a highly variable phenotype that may include intellectual disability, epilepsy, facial dysmorphism and digit anomalies. Rare patients carrying homozygous deletions show more severe phenotypes including epileptic encephalopathy, hypotonia and poor growth. For years, CHRNA7 (MIM: 118511), was considered the candidate gene that could account for this syndrome. However, recent studies in mouse models have shown that OTUD7A/CEZANNE2 (MIM: 612024), which encodes for an ovarian tumor (OTU) deubiquitinase, should be considered the critical gene responsible for brain dysfunction. In this study, a patient presenting with severe global developmental delay, language impairment and epileptic encephalopathy was referred to our genetics center. Trio exome sequencing (tES) analysis identified a homozygous OTUD7A missense variant (NM_130901.2:c.697C>T), predicted to alter an ultraconserved amino acid, p.(Leu233Phe), lying within the OTU catalytic domain. Its subsequent segregation analysis revealed that the parents, presenting with learning disability, and brother were heterozygous carriers. Biochemical assays demonstrated that proteasome complex formation and function were significantly reduced in patient‐derived fibroblasts and in OTUD7A knockout HAP1 cell line. We provide evidence that biallelic pathogenic OTUD7A variation is linked to early‐onset epileptic encephalopathy and proteasome dysfunction. [ABSTRACT FROM AUTHOR]

Published

2020

17. Vps13b is required for acrosome biogenesis through functions in Golgi dynamic and membrane trafficking.

Author

Da Costa, Romain, Bordessoules, Morgane, Guilleman, Magali, Carmignac, Virginie, Lhussiez, Vincent, Courot, Hortense, Bataille, Amandine, Chlémaire, Amandine, Bruno, Céline, Fauque, Patricia, Thauvin, Christel, Faivre, Laurence, and Duplomb, Laurence

Subjects

*GOLGI apparatus, *ORGANELLE formation, *MALE infertility, *SPERMATOZOA, *OLIGOSPERMIA

Abstract

The sperm acrosome is a lysosome-related organelle that develops using membrane trafficking from the Golgi apparatus as well as the endolysosomal compartment. How vesicular trafficking is regulated in spermatids to form the acrosome remains to be elucidated. VPS13B, a RAB6-interactor, was recently shown involved in endomembrane trafficking. Here, we report the generation of the first Vps13b-knockout mouse model and show that male mutant mice are infertile due to oligoasthenoteratozoospermia. This phenotype was explained by a failure of Vps13b deficient spermatids to form an acrosome. In wild-type spermatids, immunostaining of Vps13b and Rab6 revealed that they transiently locate to the acrosomal inner membrane. Spermatids lacking Vps13b did not present with the Golgi structure that characterizes wild-type spermatids and showed abnormal targeting of PNA- and Rab6-positive Golgi-derived vesicles to Eea1- and Lamp2-positive structures. Altogether, our results uncover a function of Vps13b in the regulation of the vesicular transport between Golgi apparatus, acrosome, and endolysosome. [ABSTRACT FROM AUTHOR]

Published

2020

18. Characterization of Vps13b-mutant mice reveals neuroanatomical and behavioral phenotypes with females less affected.

Author

Montillot, Charlotte, Skutunova, Emilia, Ayushma, Dubied, Morgane, Lahmar, Adam, Nguyen, Sylvie, Peerally, Benazir, Prin, Fabrice, Duffourd, Yannis, Thauvin-Robinet, Christel, Duplomb, Laurence, Wang, Heng, Ansar, Muhammad, Faivre, Laurence, Navarro, Nicolas, Minocha, Shilpi, Collins, Stephan C., and Yalcin, Binnaz

Subjects

*DENTATE gyrus, *CINGULATE cortex, *BRAIN anatomy, *PHENOTYPES, *MOTOR cortex

Abstract

The vacuolar protein sorting-associated protein 13B (VPS13B) is a large and highly conserved protein. Disruption of VPS13B causes the autosomal recessive Cohen syndrome, a rare disorder characterized by microcephaly and intellectual disability among other features, including developmental delay, hypotonia, and friendly-personality. However, the underlying mechanisms by which VPS13B disruption leads to brain dysfunction still remain unexplained. To gain insights into the neuropathogenesis of Cohen syndrome, we systematically characterized brain changes in Vps13b -mutant mice and compared murine findings to 235 previously published and 17 new patients diagnosed with VPS13B -related Cohen syndrome. We showed that Vps13b is differentially expressed across brain regions with the highest expression in the cerebellum, the hippocampus and the cortex with postnatal peak. Half of the Vps13b −/− mice die during the first week of life. The remaining mice have a normal lifespan and display the core phenotypes of the human disease, including microcephaly, growth delay, hypotonia, altered memory, and enhanced sociability. Systematic 2D and 3D brain histo-morphological analyses reveal specific structural changes in the brain starting after birth. The dentate gyrus is the brain region with the most prominent reduction in size, while the motor cortex is specifically thinner in layer VI. The fornix, the fasciculus retroflexus, and the cingulate cortex remain unaffected. Interestingly, these neuroanatomical changes implicate an increase of neuronal death during infantile stages with no progression in adulthood suggesting that VPS13B promotes neuronal survival early in life. Importantly, whilst both sexes were affected, some neuroanatomical and behavioral phenotypes were less pronounced or even absent in females. We evaluate sex differences in Cohen patients and conclude that females are less affected both in mice and patients. Our findings provide new insights about the neurobiology of VPS13B and highlight previously unreported brain phenotypes while defining Cohen syndrome as a likely new entity of non-progressive infantile neurodegeneration. • VPS13B has many roles in various developmental contexts • VPS13B controls brain anatomy and behavior • VPS13B promotes the survival of neurons after birth • VPS13B has a more important role in males than females [ABSTRACT FROM AUTHOR]

Published

2023

19. Changing facial phenotype in Cohen syndrome: towards clues for an earlier diagnosis.

Author

El Chehadeh-Djebbar, Salima, Blair, Edward, Holder-Espinasse, Muriel, Moncla, Anne, Frances, Anne-Marie, Rio, Marlène, Debray, François-Guillaume, Rump, Patrick, Masurel-Paulet, Alice, Gigot, Nadège, Callier, Patrick, Duplomb, Laurence, Aral, Bernard, Huet, Frédéric, Thauvin-Robinet, Christel, and Faivre, Laurence

Subjects

*SYNDROMES, *PHENOTYPES, *FACE, *DIAGNOSIS, *PRESCHOOL children

Abstract

Cohen syndrome (CS) is a rare autosomal recessive condition caused by mutations and/or large rearrangements in the VPS13B gene. CS clinical features, including developmental delay, the typical facial gestalt, chorioretinal dystrophy (CRD) and neutropenia, are well described. CS diagnosis is generally raised after school age, when visual disturbances lead to CRD diagnosis and to VPS13B gene testing. This relatively late diagnosis precludes accurate genetic counselling. The aim of this study was to analyse the evolution of CS facial features in the early period of life, particularly before school age (6 years), to find clues for an earlier diagnosis. Photographs of 17 patients with molecularly confirmed CS were analysed, from birth to preschool age. By comparing their facial phenotype when growing, we show that there are no special facial characteristics before 1 year. However, between 2 and 6 years, CS children already share common facial features such as a short neck, a square face with micrognathia and full cheeks, a hypotonic facial appearance, epicanthic folds, long ears with an everted upper part of the auricle and/or a prominent lobe, a relatively short philtrum, a small and open mouth with downturned corners, a thick lower lip and abnormal eye shapes. These early transient facial features evolve to typical CS facial features with aging. These observations emphasize the importance of ophthalmological tests and neutrophil count in children in preschool age presenting with developmental delay, hypotonia and the facial features we described here, for an earlier CS diagnosis. [ABSTRACT FROM AUTHOR]

Published

2013

20. In-Frame Mutations in Exon 1 of SKI Cause Dominant Shprintzen-Goldberg Syndrome

Author

Carmignac, Virginie, Thevenon, Julien, Adès, Lesley, Callewaert, Bert, Julia, Sophie, Thauvin-Robinet, Christel, Gueneau, Lucie, Courcet, Jean-Benoit, Lopez, Estelle, Holman, Katherine, Renard, Marjolijn, Plauchu, Henri, Plessis, Ghislaine, De Backer, Julie, Child, Anne, Arno, Gavin, Duplomb, Laurence, Callier, Patrick, Aral, Bernard, and Vabres, Pierre

Subjects

*VELOCARDIOFACIAL syndrome, *GENETIC mutation, *EXONS (Genetics), *HETEROZYGOSITY, *DELETION mutation, *NUCLEOTIDE sequence

Abstract

Shprintzen-Goldberg syndrome (SGS) is characterized by severe marfanoid habitus, intellectual disability, camptodactyly, typical facial dysmorphism, and craniosynostosis. Using family-based exome sequencing, we identified a dominantly inherited heterozygous in-frame deletion in exon 1 of SKI. Direct sequencing of SKI further identified one overlapping heterozygous in-frame deletion and ten heterozygous missense mutations affecting recurrent residues in 18 of the 19 individuals screened for SGS; these individuals included one family affected by somatic mosaicism. All mutations were located in a restricted area of exon 1, within the R-SMAD binding domain of SKI. No mutation was found in a cohort of 11 individuals with other marfanoid-craniosynostosis phenotypes. The interaction between SKI and Smad2/3 and Smad 4 regulates TGF-β signaling, and the pattern of anomalies in Ski-deficient mice corresponds to the clinical manifestations of SGS. These findings define SGS as a member of the family of diseases associated with the TGF-β-signaling pathway. [Copyright &y& Elsevier]

Published

2012

21. Glycosaminoglycans inhibit the adherence and the spreading of osteoclasts and their precursors: Role in osteoclastogenesis and bone resorption

Author

Baud’huin, Marc, Ruiz-Velasco, Carmen, Jego, Gaëtan, Charrier, Céline, Gasiunas, Nijole, Gallagher, John, Maillasson, Mike, Naggi, Annamaria, Padrines, Marc, Redini, Françoise, Duplomb, Laurence, and Heymann, Dominique

Subjects

*GLYCOSAMINOGLYCANS, *CELL adhesion, *OSTEOCLASTS, *BONE resorption, *OLIGOSACCHARIDES, *HEPARIN

Abstract

Abstract: The bone microenvironment (e.g. glycosaminoglycans (GAGs), growth factors) plays a major role in bone resorption, especially in the formation of osteoclasts which differentiate from the hematopoietic lineage in the presence of RANKL. Previous studies revealed that GAGs may influence osteoclastogenesis, but data are very controversial, some studies showing an inhibitory effect of GAGs on osteoclastic differentiation whereas others demonstrated a stimulatory effect. To clarify their activities, we investigated the effect of 5 families of GAGs in three different models of human/mouse osteoclastogenesis. The present data revealed that heparin inhibited osteoclastogenesis in these three models, which was confirmed by a decrease in mRNA expression of osteoclastic markers and by an inhibition of the bone resorption capacity. We also demonstrated in RAW 264.7 cells that other families of GAGs different from heparin inhibited RANKL-induced osteoclastogenesis, and that this inhibition was dependent on the length and the level of sulfation of GAGs. In the present work, heparin did not bind to RANKL and did not modulate RANKL signaling. Heparin acted at 2 distinct steps of osteoclastogenesis from human CD14+ cells: first, heparin strongly decreased the adherence of osteoclast precursors, and secondly inhibited osteoclasts to spread and to be active. Furthermore, the second action of heparin was reversible as the removal of heparin at the end of the culture time allowed the condensed cells to spread out and showed the formation of morphological active osteoclasts. The present work clearly evidences that GAGs inhibit osteoclastogenesis in vitro and strengthens the therapeutic interest of defined GAGs in osteolytic diseases. [ABSTRACT FROM AUTHOR]

Published

2011

22. Gallium modulates osteoclastic bone resorption in vitro without affecting osteoblasts.

Author

Verron, Elise, Masson, Martial, Khoshniat, Solmaz, Duplomb, Laurence, Wittrant, Yohann, Baud'huin, Marc, Badran, Zahi, Bujoli, Bruno, Janvier, Pascal, Scimeca, Jean-Claude, Bouler, Jean-Michel, and Guicheux, Jérôme

Subjects

*OSTEOCLASTS, *BONE resorption, *GALLIUM, *BONE diseases, *HYPERCALCEMIA, *OSTEITIS deformans, *BONE cells

Abstract

Background and purpose: Gallium (Ga) has been shown to be effective in the treatment of disorders associated with accelerated bone loss, including cancer-related hypercalcemia and Paget's disease. These clinical applications suggest that Ga could reduce bone resorption. However, few studies have studied the effects of Ga on osteoclastic resorption. Here, we have explored the effects of Ga on bone cells in vitro. Experimental approach: In different osteoclastic models [osteoclasts isolated from long bones of neonatal rabbits (RBC), murine RAW 264.7 cells and human CD14-positive cells], we have performed resorption activity tests, staining for tartrate resistant acid phosphatase (TRAP), real-time polymerase chain reaction analysis, viability and apoptotic assays. We also evaluated the effect of Ga on osteoblasts in terms of proliferation, viability and activity by using an osteoblastic cell line (MC3T3-E1) and primary mouse osteoblasts. Key results: Gallium dose-dependently (0-100 µM) inhibited the in vitro resorption activity of RBC and induced a significant decrease in the expression level of transcripts coding for osteoclastic markers in RAW 264.7 cells. Ga also dramatically reduced the formation of TRAP-positive multinucleated cells. Ga down-regulated in a dose-dependant manner the expression of the transcription factor NFATc1. However, Ga did not affect the viability or activity of primary and MC3T3-E1 osteoblasts. Conclusions and implications: Gallium exhibits a dose-dependent anti-osteoclastic effect by reducing in vitro osteoclastic resorption, differentiation and formation without negatively affecting osteoblasts. We provide evidence that this inhibitory mechanism involves down-regulation of NFATc1 expression, a master regulator of RANK-induced osteoclastic differentiation. [ABSTRACT FROM AUTHOR]

Published

2010

23. Long term oncostatin M treatment induces an osteocyte-like differentiation on osteosarcoma and calvaria cells

Author

Brounais, Bénédicte, David, Emmanuelle, Chipoy, Céline, Trichet, Valérie, Ferré, Virginie, Charrier, Céline, Duplomb, Laurence, Berreur, Martine, Rédini, Françoise, Heymann, Dominique, and Blanchard, Frédéric

Subjects

*INTERLEUKIN-6, *OSTEOSARCOMA, *CELL differentiation, *CALVARIA, *APOPTOSIS, *LABORATORY rats, *ANTINEOPLASTIC agents, *OSTEOCYTES, *THERAPEUTICS

Abstract

Abstract: Previous in vitro studies on primary osteoblastic and osteosarcoma cells (normal and transformed osteoblasts) have shown that oncostatin M (OSM), a member of the interleukin-6 family, possesses cytostatic and pro-apoptotic effects in association with complex and poorly understood activities on osteoblast differentiation. In this study, we use rat osteosarcoma cells transduced with lentiviral particles encoding OSM (lvOSM) to stably produce this cytokine. We show that after several weeks of culture, transduced OSRGA and ROS 17/2.8 cells are growth inhibited and sensitized to apoptosis induced by the kinase inhibitor Staurosporine (Sts). Moreover, this long term OSM treatment induces (i) a decrease in osteoblastic markers, (ii) morphological changes leading to an elongated and/or stellate shape and (iii) an increase in osteocytic markers (sclerostin and/or E11), suggesting an osteocyte-like differentiation. We also show that non transformed rat calvaria cells transduced with lvOSM differentiate into stellate shaped cells expressing sclerostin, E11, Phex and functional hemichannels. Together, these results indicate that osteosarcoma cells stably producing OSM do not develop resistance to this cytokine and thus could be a valuable new tool to study the anti-cancer effect of OSM in vivo. Moreover, OSM-over-expressing osteoblastic cells differentiate into osteocyte-like cells, the major cellular contingent in bone, providing new culture conditions for this cell type which is difficult to obtain in vitro. [Copyright &y& Elsevier]

Published

2009

24. FR901228, an inhibitor of histone deacetylases, increases the cellular responsiveness to IL-6 type cytokines by enhancing the expression of receptor proteins.

Author

Blanchard, Fréderic, Kinzie, Erin, Yanping Wang, Duplomb, Laurence, Godard, Anne, Held, Wiiliam A., Asch, Bonnie B., and Baumann, Heinz

Subjects

*HISTONE deacetylase, *INTERLEUKIN-6, *CYTOKINES, *CANCER cells

Abstract

Presents a study which demonstrated that treatment with FR901228, an inhibitor of histome deacetylases, increases cellular responsiveness to interleukin-6 type cytokines in different cell types, including normal fibroblasts and tumor cell lines. Materials and methods; Results; Discussion.

Published

2002

25. Extracellular HSP110 skews macrophage polarization in colorectal cancer.

Author

Berthenet, Kevin, Boudesco, Christophe, Collura, Ada, Svrcek, Magali, Richaud, Sarah, Hammann, Arlette, Causse, Sebastien, Yousfi, Nadhir, Wanherdrick, Kristell, Duplomb, Laurence, Duval, Alex, Garrido, Carmen, and Jego, Gaetan

Subjects

*COLON cancer, *MACROPHAGES, *EXTRACELLULAR matrix, *MICROSATELLITE repeats, *SMALL interfering RNA

Abstract

HSP110 is induced by different stresses and, through its anti-apoptotic and chaperoning properties, helps the cells to survive these adverse situations. In colon cancers, HSP110 is abnormally abundant. We have recently showed that colorectal cancer (CRC) patients with microsatellite instability (MSI) had an improved response to chemotherapy because they harbor an HSP110 inactivating mutation (HSP110DE9). In this work, we have used patients' biopsies and human CRC cells grownin vitroandin vivo(xenografts) to demonstrate that (1) HSP110 is secreted by CRC cells and that the amount of this extracellular HSP110 is strongly decreased by the expression of the mutant HSP110DE9, (2) Supernatants from CRC cells overexpressing HSP110 or purified recombinant human HSP110 (LPS-free) affect macrophage differentiation/polarization by favoring a pro-tumor, anti-inflammatory profile, (3) Conversely, inhibition of HSP110 (expression of siRNA, HSP110DE9 or immunodepletion) induced the formation of macrophages with a cytotoxic, pro-inflammatory profile. (4) Finally, this effect of extracellular HSP110 on macrophages seems to implicate TLR4. These results together with the fact that colorectal tumor biopsies with HSP110 high were infiltrated with macrophages with a pro-tumoral profile while those with HSP110 low were infiltrated with macrophages with a cytotoxic profile, suggest that the effect of extracellular HSP110 function on macrophages may also contribute to the poor outcomes associated with HSP110 expression. [ABSTRACT FROM AUTHOR]

Published

2016

26. Interleukin-34 is expressed by giant cell tumours of bone and plays a key role in RANKL-induced osteoclastogenesis

Author

Baud'huin, Marc, Renault, Romain, Charrier, Céline, Riet, Anne, Brion, Régis, Moreau, Anne, Gouin, Francois, Duplomb, Laurence, and Heymann, Dominique

Published

2010