Your search keyword '"Camoin, Luc"' showing total 18 results

1. Recognition of human proinsulin leader sequence by class I-restricted T-cells in HLA-A*0201 transgenic mice and in human type 1 diabetes

Author

Toma, Andrea, Laika, Taghrid, Haddouk, Samy, Luce, Sandrine, Briand, Jean-Paul, Camoin, Luc, Connan, Francine, Lambert, Marion, Caillat-Zucman, Sophie, Carel, Jean-Claude, Muller, Sylviane, Choppin, Jeannine, Lemonnier, Francois, and Boitard, Christian

Subjects

T cells -- Health aspects -- Research -- Genetic aspects, Antigenic determinants -- Health aspects -- Research -- Genetic aspects, Type 1 diabetes -- Care and treatment -- Genetic aspects -- Research, Proinsulin -- Health aspects -- Research -- Genetic aspects, Health, Care and treatment, Research, Genetic aspects, Health aspects

Abstract

OBJECTIVE--A restricted region of proinsulin located in the B chain and adjacent region of C-peptide has been shown to contain numerous candidate epitopes recognized by [CD8.sup.+] T-cells. Our objective is to characterize HLA class I-restricted epitopes located within the preproinsulin leader sequence. RESEARCH DESIGN AND METHODS--Seven 8- to 11-mer preproinsulin peptides carrying anchoring residues for HLA-A1, -A2, -A24, and -B8 were selected from databases. HLA-A2-restricted peptides were tested for immunogenicity in transgenic mice expressing a chimeric HLA-A*0201/β2-microglobulin molecule. The peptides were studied for binding to purified HLA class I molecules, selected for carrying COOH-terminal residues generated by proteasome digestion in vitro and tested for recognition by human lymphocytes using an ex vivo interferon-γ (IFN-γ) ELISpot assay. RESULTS--Five HLA-A2-restricted peptides were immunogenic in transgenic mice. Murine T-cell clones specific for these peptides were cytotoxic against cells transfected with the preproinsulin gene. They were recognized by peripheral blood mononuclear cells (PBMCs) from 17 of 21 HLA-A2 type 1 diabetic patients. PBMCs from 25 of 38 HLA-A1, -A2, -A24, or -B8 patients produced IFN-γ in response to six preproinsulin peptides covering residues 2-25 within the preproinsulin region. In most patients, the response was against several class I-restricted peptides. T-cells recognizing preproinsulin peptide were characterized as [CD8.sup.+] T-cells by staining with peptide/ HLA-A2 tetramers. CONCLUSIONS--We defined class I-restricted epitopes located within the leader sequence of human preproinsufin through in vivo (transgenic mice) and ex vivo (diabetic patients) assays, illustrating the possible role of preproinsulin-specific [CD8.sup.+] T-cells in human type 1 diabetes., Type 1 diabetes involves the activation of lympho1 cytes against β-cell autoantigens. In animals, the predominant role of T-cells is supported by experiments in which diabetes is transferred by diabetogenic [...]

Published

2009

2. Mutations in the human leptin and leptin receptor genes as models of serum leptin receptor regulation

Author

Lahlou, Najiba, Issad, Tarik, Lebouc, Yves, Carel, Jean-Claude, Camoin, Luc, Roger, Marc, and Girard, Jean

Subjects

Genetic disorders -- Research -- Genetic aspects, Diabetes -- Research, Leptin -- Genetic aspects -- Research, Health, Genetic aspects, Research

Abstract

A part of serum Ob leptin, an adipocyte-secreted peptide, is bound to a soluble Ob receptor (sObR). Immunoreactive sObR was measured in 125 lean or obese control subjects (group 1), 18 individuals with a mutation in the leptin gene impairing leptin secretion (group 2), and 10 individuals with a mutation in the ObR gene, leading to production of a truncated ObR not anchored to cell membranes (group 3). In group 1, sObR levels were negatively correlated with age and BMI in children and with BMI in adults, sObR levels were also negatively correlated with leptin levels. Leptin binding activity and sObR levels coeluted in gel-filtration chromatography. In group 2, sObR levels did not differ from those in lean control subjects and were not correlated with BMI. A single peak was detected in chromatographic fractions. In group 3, sObR levels were high and positively correlated with BMI. Immunoreactive sObR coeluted with leptin binding activity. These data demonstrate that leptin is not needed for ObR gene expression, and they suggest that leptin plays a role in receptor downregulation because sObR levels are negatively correlated with leptin levels and BMI in control subjects, whereas sObR levels are not depressed in obese leptin-deficient or leptin receptor-deficient individuals. Diabetes 51:1980-1985, 2002, Leptin exerts its biological activity through a membrane receptor (ObR) located in various tissues, including the brain (rev. in 1). The lack of leptin due to mutations in the leptin [...]

Published

2002

3. The Scribble family in cancer: twentieth anniversary

Author

Santoni, Marie-Josée, Kashyap, Rudra, Camoin, Luc, and Borg, Jean-Paul

Abstract

Among the more than 160 PDZ containing proteins described in humans, the cytoplasmic scaffold Scribble stands out because of its essential role in many steps of cancer development and dissemination. Its fame has somehow blurred the importance of homologous proteins, Erbin and Lano, all belonging to the LRR and PDZ (LAP) protein family first described twenty years ago. In this review, we will retrace the history of LAP family protein research and draw attention to their contribution in cancer by detailing the features of its members at the structural and functional levels, and highlighting their shared—but also different—implication in the tumoral process.

Published

2020

4. The scaffolding function of the RLTPR protein explains its essential role for CD28 co-stimulation in mouse and human T cells

Author

Roncagalli, Romain, Cucchetti, Margot, Jarmuzynski, Nicolas, Grégoire, Claude, Bergot, Elise, Audebert, Stéphane, Baudelet, Emilie, Menoita, Marisa Goncalves, Joachim, Anais, Durand, Stéphane, Suchanek, Miloslav, Fiore, Frédéric, Zhang, Lichen, Liang, Yinming, Camoin, Luc, Malissen, Marie, and Malissen, Bernard

Abstract

The RLTPR cytosolic protein, also known as CARMIL2, is essential for CD28 co-stimulation in mice, but its importance in human T cells and mode of action remain elusive. Here, using affinity purification followed by mass spectrometry analysis, we showed that RLTPR acts as a scaffold, bridging CD28 to the CARD11/CARMA1 cytosolic adaptor and to the NF-κB signaling pathway, and identified proteins not found before within the CD28 signaling pathway. We further demonstrated that RLTPR is essential for CD28 co-stimulation in human T cells and that its noncanonical pleckstrin-homology domain, leucine-rich repeat domain, and proline-rich region were mandatory for that task. Although RLTPR is thought to function as an actin-uncapping protein, this property was dispensable for CD28 co-stimulation in both mouse and human. Our findings suggest that the scaffolding role of RLTPR predominates during CD28 co-stimulation and underpins the similar function of RLTPR in human and mouse T cells. Along that line, the lack of functional RLTPR molecules impeded the differentiation toward Th1 and Th17 fates of both human and mouse CD4+ T cells. RLTPR was also expressed in both human and mouse B cells. In the mouse, RLTPR did not play, however, any detectable role in BCR-mediated signaling and T cell-independent B cell responses.

Published

2016

5. Src-family-tyrosine kinase Lyn is critical for TLR2-mediated NF-κB activation through the PI 3-kinase signaling pathway

Author

Toubiana, Julie, Rossi, Anne-Lise, Belaidouni, Nadia, Grimaldi, David, Pene, Frederic, Chafey, Philippe, Comba, Béatrice, Camoin, Luc, Bismuth, Georges, Claessens, Yann-Erick, Mira, Jean-Paul, and Chiche, Jean-Daniel

Abstract

TLR2 has a prominent role in host defense against a wide variety of pathogens. Stimulation of TLR2 triggers MyD88-dependent signaling to induce NF-κB translocation, and activates a Rac1-PI 3-kinase dependent pathway that leads to transactivation of NF-κB through phosphorylation of the P65 NF-κB subunit. This transactivation pathway involves tyrosine phosphorylations. The role of the tyrosine kinases in TLR signaling is controversial, with discrepancies between studies using only chemical inhibitors and knockout mice. Here, we show the involvement of the tyrosine-kinase Lyn in TLR2-dependent activation of NF-κB in human cellular models, by using complementary inhibition strategies. Stimulation of TLR2 induces the formation of an activation cluster involving TLR2, CD14, PI 3-kinase and Lyn, and leads to the activation of AKT. Lyn-dependent phosphorylation of the p110 catalytic subunit of PI 3-kinase is essential to the control of PI 3-kinase biological activity upstream of AKT and thereby to the transactivation of NF-κB. Thus, Lyn kinase activity is crucial in TLR2-mediated activation of the innate immune response in human mononuclear cells.

Published

2015

6. CD9 mediates the uptake of extracellular vesicles from cancer-associated fibroblasts that promote pancreatic cancer cell aggressiveness

Author

Nigri, Jérémy, Leca, Julie, Tubiana, Sarah-Simha, Finetti, Pascal, Guillaumond, Fabienne, Martinez, Sébastien, Lac, Sophie, Iovanna, Juan L., Audebert, Stéphane, Camoin, Luc, Vasseur, Sophie, Bertucci, François, and Tomasini, Richard

Abstract

In pancreatic ductal adenocarcinoma (PDAC), signaling from stromal cells is implicated in metastatic progression. Tumor-stroma cross-talk is often mediated through extracellular vesicles (EVs). We previously reported that EVs derived from cancer-associated stromal fibroblasts (CAFs) that are abundant in annexin A6 (ANXA6+EVs) support tumor cell aggressiveness in PDAC. Here, we found that the cell surface glycoprotein and tetraspanin CD9 is a key component of CAF-derived ANXA6+EVs for mediating this cross-talk. CD9 was abundant on the surface of ANXA6+CAFs isolated from patient PDAC samples and from various mouse models of PDAC. CD9 colocalized with CAF markers in the tumor stroma, and CD9 abundance correlated with tumor stage. Blocking CD9 impaired the uptake of ANXA6+EVs into cultured PDAC cells. Signaling pathway arrays and further analyses revealed that the uptake of CD9+ANXA6+EVs induced mitogen-activated protein kinase (MAPK) pathway activity, cell migration, and epithelial-to-mesenchymal transition (EMT). Blocking either CD9 or p38 MAPK signaling impaired CD9+ANXA6+EV–induced cell migration and EMT in PDAC cells. Analysis of bioinformatic datasets indicated that CD9 abundance was an independent marker of poor prognosis in patients with PDAC. Our findings suggest that CD9-mediated stromal cell signaling promotes PDAC progression.

Published

2022

7. Identification of New Mechanisms of Cellular Response to Chemotherapy by Tracking Changes in Post-Translational Modifications by Ubiquitin and Ubiquitin-Like Proteins

Author

Bonacci, Thomas, Audebert, Stéphane, Camoin, Luc, Baudelet, Emilie, Bidaut, Ghislain, Garcia, Maxime, Witzel, Ini-Isabée, Perkins, Neil D., Borg, Jean-Paul, Iovanna, Juan-Lucio, and Soubeyran, Philippe

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is a very aggressive malignancy characterized by an excessive resistance to all known anticancer therapies, a still largely elusive phenomenon. To identify original mechanisms, we have explored the role of post-translational modifications (PTMs) mediated by members of the ubiquitin family. Although alterations of these pathways have been reported in different cancers, no methodical search for these kinds of anomalies has been performed so far. Therefore, we studied the ubiquitin-, Nedd8-, and SUMO1-specific proteomes of a pancreatic cancer cell line (MiaPaCa-2) and identified changes induced by gemcitabine, the standard PDAC’s chemotherapeutic drug. These PTMs profiles contained both known major substrates of all three modifiers as well as original ones. Gemcitabine treatment altered the PTM profile of proteins involved in various biological functions, some known cancer associated genes, many potentially cancer-associated genes, and several cancer-signaling networks, including canonical and noncanonical WNT and PI3K/Akt/MTOR pathways. Some of these altered PTMs formed groups of functionally and physically associated proteins. Importantly, we could validate the gemcitabine-induced PTMs variations of relevant candidates and we could demonstrate the biological significance of such altered PTMs by studying in detail the sumoylation of SNIP1, one of these new targets.

Published

2014

8. Essential and nonredundant roles for Diaphanous formins in cortical microtubule capture and directed cell migration

Author

Daou, Pascale, Hasan, Salma, Breitsprecher, Dennis, Baudelet, Emilie, Camoin, Luc, Audebert, Stéphane, Goode, Bruce L., and Badache, Ali

Abstract

The Diaphanous formins mDia1, mDia2, and mDia3 are involved in the capture of cortical microtubules and ErbB2-dependent directed migration. These functions are independent of actin. They are mediated by mDia FH2 domains, which associate with distinct sets of proteins. Rab6IP2 is a novel interactor of mDia1 that contributes to microtubule tethering.

Published

2014

9. A Generic Approach for the Purification of Signaling Complexes That Specifically Interact with the Carboxyl-terminal Domain of G Protein-coupled Receptors

Author

Maurice, Pascal, Daulat, Avais M., Broussard, Cédric, Mozo, Julien, Clary, Guilhem, Hotellier, Françoise, Chafey, Philippe, Guillaume, Jean-Luc, Ferry, Gilles, Boutin, Jean A., Delagrange, Philippe, Camoin, Luc, and Jockers, Ralf

Abstract

G protein-coupled receptors (GPCRs) constitute the largest family of membrane receptors and are major drug targets. Recent progress has shown that GPCRs are part of large protein complexes that regulate their activity. We present here a generic approach for identification of these complexes that is based on the use of receptor subdomains and that overcomes the limitations of currently used genetics and proteomics approaches. Our approach consists of a carefully balanced combination of chemically synthesized His6-tagged baits, immobilized metal affinity chromatography, one- and two-dimensional gel electrophoresis separation and mass spectrometric identification. The carboxyl-terminal tails (C-tails) of the human MT1and MT2melatonin receptors, two class A GPCRs, were used as models to purify protein complexes from mouse brain lysates. We identified 32 proteins that interacted with the C-tail of MT1, 14 proteins that interacted with the C-tail of MT2, and eight proteins that interacted with both C-tails. Several randomly selected proteins were validated by Western blotting, and the functional relevance of our data was further confirmed by showing the interaction between the full-length MT1and the regulator of G protein signaling Z1 in transfected HEK 293 cells and native tissue. Taken together, we have established an integrated and generic purification strategy for the identification of high quality and functionally relevant GPCR-associated protein complexes that significantly widens the repertoire of available techniques.

Published

2008

10. Purification and Identification of Two Putative Autolytic Sites in Human Calpain 3 (p94) Expressed in Heterologous Systems

Author

Federici, Christian, Eshdat, Yuval, Richard, Isabelle, Bertin, Brigitte, Guillaume, Jean Luc, Hattab, Maurice, Beckmann, Jacques S., Strosberg, A.Donny, and Camoin, Luc

Abstract

Human muscle-specific calpain (CAPN3) was expressed in two heterologous systems: Sf9 insect cells andEscherichia colicells. Polyclonal antibodies were prepared against peptides whose sequences were taken from the three unique regions of human CAPN3, namely NS, IS1, and IS2, which are not found in other members of the calpain family. Western blot analysis using these antibodies revealed that CAPN3 was well expressed in both systems. However, considerable rapid degradation of the expressed CAPN3 was observed in both Sf9 andE. colicells. These antibodies were therefore also used to detect CAPN3 and its degradation products in human and rat muscles, as well as to detect the protein throughout the purification of the recombinant His-tagged human CAPN3 by Ni2+affinity chromatography and by immunopurification over immobilized antibody. An alternative purification procedure was used for purification of all putative CAPN3 immunoreactive fragments by combining SDS–PAGE and hydroxyapatite chromatography. Two fragments of CAPN3 of approximately 55 kDa were purified, and their N-terminal amino acid sequencing demonstrated that cleavage of CANP3 occurred between residues 30–31 and 412–413, thus providing the first evidence for the localization of putative autolytic sites in this enzyme.

Published

1999

11. Human preformed IgG combining with membrane-bound porcine serotransferrin lyse porcine endothelial cells through antibody-dependent cellular cytotoxicity

Author

Atia, Nathalie, Camoin, Luc, Duflos, Guillaume, Malassagne, Benoît, Chéreau, Christiane, Filipponi, Franco, Mahboub, Saïd, Batteux, Frédéric, Conti, Filomena, Michalski, Jean-Claude, Houssin, Didier, Calmus, Yvon, and Weill, Bernard

Abstract

Preformed antibodies are involved in xenograft rejection. The purpose of this work was to characterize porcine xenoantigens recognized by human preformed IgG (hpIgG), and to investigate the role of hpIgG in xenogeneic rejection. IgG eluted from porcine livers perfused with human plasma, human sera and total human IgG were immunoblotted on porcine aortic endothelial cell extracts. The amino acid sequence of a 76-kDa antigen constantly revealed was 100 % homologous with porcine serotransferrin (psTf). hpIgG from human sera, human IgG1 and IgG2 and F(ab ' )2 γ specifically bound to psTf. Neutralization by psTf abolished that binding. Although α1, 3-linked galactose residues (Galα1,3Gal) is the dominant epitope recognized by preformed antibodies in the swine-to-human combination, the analysis of carbohydrate composition of psTf showed that the molecule was devoid of Galα1,3Gal moieties and that preformed anti-psTf IgG bound to epitopes localized on the peptide core of the molecule. Purified human anti-psTf IgG antibodies were able to bind to psTf linked to its receptor on porcine endothelial cells, and to kill those cells through antibody-dependent cellular cytotoxicity.

Published

1998

12. Amino acid sequence and three‐dimensional structure of the Tn‐specific isolectin B4 from Vicia villosa

Author

Osinaga, Eduardo, Tello, Diana, Batthyany, Carlos, Bianchet, Mario, Tavares, Gisele, Durán, Rosario, Cerveñansky, Carlos, Camoin, Luc, Roseto, Alberto, and Alzari, Pedro M

Abstract

The partial amino acid sequence of the tetrameric isolectin B4 from Vicia villosaseeds has been determined by peptide analysis, and its three‐dimensional structure solved by molecular replacement techniques and refined at 2.9 Å resolution to a crystallographic R‐factor of 21%. Each subunit displays the thirteen‐stranded β‐barrel topology characteristic of legume lectins. The amino acid residues involved in metal‐ and sugar‐binding are similar to those of other GalNAc‐specific lectins, indicating that residues outside the carbohydrate‐binding pocket modulate the affinity for the Tn glycopeptide. Isolectin B4 displays an unusual quaternary structure, probably due to protein glycosylation.

Published

1997

13. Purification and Characterization of Equine Testicular Cytochrome P-450 Aromatase: Comparison with the Human Enzyme

Author

Moslemi, Safa, Vibet, Alain, Papadopoulos, Vassilios, Camoin, Luc, Silberzahn, Pierre, and Gaillard, Jean-Luc

Abstract

Cytochrome P-450 aromatase was purified by five chromatographic steps from adult stallion testis. It was first separated from NADPH-cytochrome P-450 reductase (reductase) on ω-aminohexyl-Sepharose 4B then purified to homogeneity on concanavalin A-Sepharose 4B, hydroxyapatite-Sepharose 4B, DEAE-Sepharose CL-6B and on a second hydroxyapatite-Sepharose 4B. On the other hand, purifications of the equine testicular and rat liver reductases, which allowed the reconstitution of aromatase activity in vitro, were achieved for each species in one chromatographic step on an adenosine 2′,5′-diphosphate-agarose affinity column. Analysis on SDS/PAGE indicated single bands with apparent molecular masses of 53, 82, and 80 kDa for purified equine testicular cytochrome P-450 aromatase (eAROM), equine testicular reductase and rat liver reductase respectively. eAROM shows a time- and concentration-dependent activity that was stable for at least 2 months when stored at −78°C. It is a highly hydrophobic protein composed from 505 residues and direct sequencing of its N-terminal part showed good homology when compared with human aromatase. When deglycosylated by N-glycosidase-F the apparent molecular mass of eAROM was decreased from 53 to 51 kDa as revealed by electrophoresis, its activity, however, was not impaired. eAROM exhibits much higher affinity for androgens than for 19-norandrogens, Km values were approximately 3, 16 and 170 nM for androstenedione (A), testosterone (T) and 19-nortestosterone (19-NT) respectively. However, it aromatizes 19-norandrostenedione (19-NA) slightly more efficiently than A, the estrone (E1) formed was 4.27 vs 3.54 pmol min−1μg−1respectively (P< 0.01). After incubation of eAROM with radiolabelled A and separation of steroids on HPLC, E1, 19-hydroxyandrostenedione (19-OHA) and 19-oxoandrostenedione (19-oxoA) were accumulated in the incubation medium in a time-dependent manner. The presence of 4-hydroxyandrostenedione (4-OHA), a suicide inhibitor of aromatase, cause a time-dependent inactivation of the enzyme. Whereas the activity of eAROM was unchanged in the presence of K+(up to 250 mM), it was increased in the presence of EDTA (up to 50 mM) and decreased in the presence of DTT or Mg2+(from 25 mM). We conclude that: (a) eAROM is a glycoprotein, however, deglycosylation by N-glycosidase-F does not appear to impair its activity, (b) eAROM aromatizes really both androgens and 19-norandrogens having a higher affinity for androgens, (c) the intermediary compounds of aromatization 19-OHA and 19-oxoA appear to be synthesized by the same active site that synthesizes E1as the final product, (d) the inhibition of eAROM by increasing concentrations of Mg2+and the stimulation of its activity by EDTA, taken together, indicate the importance of negatively charged residues in the polypeptide chain of equine aromatase, which play a role in enzymatic activity.

Published

1997

14. Characterization of a Novel Iodocyanopindolol and SM-11044 Binding Protein, Which May Mediate Relaxation of Depolarized Rat Colon Tonus*

Author

Sugasawa, Toshinari, Matsuzaki-Fujita, Masago, Guillaume, Jean-Luc, Camoin, Luc, Morooka, Shigeaki, and Strosberg, A. Donny

Abstract

Studies under blockade of α-, β1-, and β2-adrenoreceptors revealed a good correlation between the responses of rat colon relaxation of depolarized tonus and of rat adipocyte lipolysis elicited by catecholamines or BRL-37344, a selective β3-adrenoreceptor agonist, suggesting β3-adrenoreceptor stimulation. In contrast, SM-11044, a nonselective β-adrenoreceptor agonist, stimulated colon relaxation more efficiently than lipolysis; its effects were differently antagonized by cyanopindolol withpA2values of 8.31 in colon and of 7.32 in adipocytes. Binding studies in rat colon smooth muscle membranes using [125I]iodocyanopindolol under blockade of adrenaline and serotonin receptors revealed the existence of a single class of sites (Kd= 11.0 nm,Bmax= 716.7 fmol/mg protein). The specific binding was saturable and reversible and was displaced by SM-11044 but not by BRL-37344, isoproterenol, noradrenaline, adrenaline, serotonin, nor dopamine. This binding site was photoaffinity labeled using [125I]iodocyanopindolol-diazirine. The labeling was prevented by SM-11044 but not by BRL-37344.

Published

1997

15. Molecular characterization of salt-stress-associated protein in citrus: protein and cDNA sequence homology to mammalian glutathione peroxidases

Author

Holland, Doron, Ben-Hayyim, Gozal, Faltin, Zehava, Camoin, Luc, Strosberg, A. Donny, and Eshdat, Yuval

Abstract

A gene encoding for a citrus salt-stress-associated protein (Cit-SAP) was cloned from Citrus sinensis salt-treated cell suspension. The gene, designated csa, was isolated from a cDNA expression library. The partial amino acid sequence of the protein, as well as that deduced from the nucleotide sequence of csa, revealed a considerable homology to mammalian glutathione peroxidase (GP), and to clone 6P229 from tobacco protoplasts. The increased expression of Cit-SAP in NaCl-treated cultured citrus cells and in citrus plants irrigated with saline water, and its similarity to GP, raise the possibility that one of the effects of salt stress in plants may be the increase of the level of free radicals.

Published

1993

16. Clustering as a Means To Control Nitrate Respiration Efficiency and Toxicity in Escherichia coli

Author

Bulot, Suzy, Audebert, Stéphane, Pieulle, Laetitia, Seduk, Farida, Baudelet, Emilie, Espinosa, Leon, Pizay, Marie-Camille, Camoin, Luc, and Magalon, Axel

Abstract

Most bacteria rely on the redox activity of respiratory complexes embedded in the cytoplasmic membrane to gain energy in the form of ATP and of an electrochemical gradient established across the membrane. Nevertheless, production of harmful and toxic nitric oxide by actively growing bacteria as either an intermediate or side-product of nitrate respiration challenges how homeostasis control is exerted. Here, we show that components of the nitrate electron transport chain are clustered, likely influencing the kinetics of the process. Nitric oxide production from this respiratory chain is controlled and handled through a multiprotein complex, including detoxifying systems. These findings point to an essential role of compartmentalization of respiratory components in bacterial cell growth.

Published

2019

17. A leptin missense mutation associated with hypogonadism and morbid obesity

Author

Strobel, Andreas, Issad, Tarik, Camoin, Luc, Ozata, Metin, and Strosberg, A. Donny

Published

1998

18. Identification of new autoantibody specificities directed at proteins involved in the transforming growth factor β pathway in patients with systemic sclerosis

Author

Bussone, Guillaume, Dib, Hanadi, Tamby, Mathieu, Broussard, Cedric, Federici, Christian, Woimant, Geneviève, Camoin, Luc, Guillevin, Loïc, and Mouthon, Luc

Abstract

Antinuclear antibodies (ANAs), usually detected by indirect immunofluorescence on HEp-2 cells, are identified in 90% of patients with systemic sclerosis (SSc). Thus, approximately 10% of SSc patients have no routinely detectable autoantibodies, and for 20% to 40% of those with detectable ANAs, the ANAs do not have identified specificity (unidentified ANAs). In this work, we aimed to identify new target autoantigens in SSc patients.

Published

2011