Your search keyword '"Z, Mishal"' showing total 150 results

1. Induction and suppression of delayed-type hypersensitivity to non-MHC antigens during lethal graft-versus-host reaction

Author

L L Pritchard, R Huchet, M Bruley-Rosset, N Riché, Z Mishal, and O Halle-Pannenko

Subjects

Immunology, Immunology and Allergy

Abstract

A delayed-type hypersensitivity reaction (DTH) to non-MHC Ag was detected during a lethal graft-vs-host reaction (GVH) induced by incompatibility for non-MHC Ag alone. In this model, when appropriate doses of B10.D2 bone marrow and lymphoid cells are grafted to irradiated (DBA/2 x B10.D2)F1 recipients, the ensuing GVH, directed against those DBA/2 non-MHC Ag absent from the B10.D2 background, results in virtually 100% mortality in less than 3 mo; donor alloimmunization against the host histocompatibility Ag considerably reduces mortality, and survival rates of 80 to 100% are common. The experiments reported here show that: 1) the cell responsible for DTH induction expresses the CD4+ CD8- phenotype; 2) CD4+ cells likewise seem to play a predominant role in the pathology of lethal GVH in this genetic combination; 3) the alloimmunization protocol that abrogates mortality also abolishes GVH-associated DTH; and 4) this suppressive effect, as shown elsewhere for the protection against mortality, is mediated by CD4- CD8- "double negative" Thy-1+ CD3+ T suppressor cells. Thus, there is a good parallel between lethal GVH and its associated DTH as concerns both induction and suppression of the two phenomena, suggesting that mortality and DTH may represent different manifestations of a common underlying mechanism. Initiation of the effector phase of DTH in the adoptive transfer model seems to be dependent on the presence of a Thy-1+ double-negative cell in the transfer inoculum; the possible relationship of this double-negative cell to the Th-1-type CD4+ DTH-mediating cell recently shown to induce lethal GVH is discussed.

Published

1992

2. Abnormal fibrin clot architecture in nephrotic patients is related to hypofibrinolysis: influence of plasma biochemical modifications: a possible mechanism for the high thrombotic tendency?

Author

J P, Colle, Z, Mishal, C, Lesty, M, Mirshahi, J, Peyne, A, Baumelou, A, Bensman, J, Soria, and C, Soria

Subjects

Adult, Male, Fibrin, Microscopy, Confocal, Nephrotic Syndrome, Adolescent, Viscosity, Fibrinolysis, Thrombosis, Middle Aged, Lipids, Elasticity, Fibrinolytic Agents, Humans, Thrombophilia, Female, Gels, Porosity, Serum Albumin, Aged

Abstract

Porosity, viscoelasticity and morphological properties of plasma fibrin from 16 nephrotic patients and 16 healthy volunteers were compared. Nephrotic patients were characterized by formation of tight and rigid plasma fibrin gels which resulted in a slower rate of fibrin lysis studied either under pressure-driven permeation or diffusional transport of fibrinolytic agents. These latter findings indicated that both abnormal fibrin network conformation and abnormal fibrin fiber structure were involved in hypofibrinolysis. Albumin supplementation up to 40 mg/ml partially restored normal fibrin architecture and increased the rate of fibrinolysis in these patients. Multiparametric analysis showed that nephrotic patients were mainly characterized by a low plasma albumin level (R = -0.85), a low albumin to fibrinogen ratio (R = -0.89) and a high resistance to lysis (R = -0.82). High triglycerides level was the only plasma modification related to the slower fibrin lysis rate (R = -0.54). High fibrin rigidity (G') was the only fibrin parameter simultaneously related to the nephrotic state (R = 0.75) and the lysis resistance (R = -0.71). After eliminating the effects of age, albumin and fibrinogen levels, low fibrin porosity (Ks) and low fiber mass-length ratio (mu) were the main features of the nephrotic state. These findings are discussed in relation to both the pathophysiology of thrombotic complications in nephrotic syndrome and their pharmacological prevention.

Published

1999

3. Pharmacological remodeling of the thrombus architecture

Author

J P, Collet, G, Montalescot, J, Soria, Z, Mishal, and C, Soria

Subjects

Blood Platelets, Fibrin, Animals, Humans, Thrombosis, Platelet Aggregation Inhibitors

Published

1999

4. Structurally different anthracyclines provoke different effects on cell cycle and tumor B cell differentiation

Author

Theodore J. Lampidis, Wolf H. Fridman, Jean-Luc Teillaud, Z Mishal, H Tapiero, Janine Moncuit, and Nadège Gruel

Subjects

Time Factors, Cellular differentiation, Pirarubicin, Flow cytometry, Mice, medicine, Animals, Doxorubicin, Aclarubicin, B cell, Pharmacology, B-Lymphocytes, Antibiotics, Antineoplastic, Hybridomas, biology, medicine.diagnostic_test, Cell Cycle, Cell Differentiation, General Medicine, Neoplasms, Experimental, Cell cycle, Molecular biology, Kinetics, medicine.anatomical_structure, Biochemistry, Immunoglobulin G, biology.protein, Antibody, Cell Division, medicine.drug

Abstract

Summary Previously we have detected a stimulatory effect on immunoglobulin (IgG) synthesis when hybridoma cells were treated with doxorubicin. In order to determine whether this is a general property of anthracycline, we have selected three analogs doxorubicin (DOX), pirarubicin (THP-DOX) and aclarubicin (ACR) — which differ mainly in the methylation state of their amino sugars. Cell cycle analysis by flow cytometry and drug localization by scanning confocal microscopy were also performed. The results show that when cells (UN2 hybridoma B cells) were exposed to subtoxic doses of DOX or THP (with unmethylated amino sugars), a strong increases in IgG secretion, heavy (H) and light (L) chain synthesis and the corresponding mRNA levels were induced. Furthermore these two drugs arrested the cells in the G2/M phase of the cell cycle. In contrast, exposure to ACR (with its methylated amino sugar) at similar subtoxic doses induced a blockade of cells in the Gl phase with no increase of IgG synthesis. at the subtoxic doses used, all three drugs could still be detected in the nucleus as well as in the cytoplasm, as determined by confocal laser microscopy. Thus, the relationship between cell cycle blockade, IgG stimulation and anthracycline structure is suggested by these results. © 1998 Elsevier, Paris.

Published

1998

5. Transcriptional activation plays a role in the induction of apoptosis by transiently transfected wild-type p53

Author

E, Yonish-Rouach, V, Deguin, T, Zaitchouk, C, Breugnot, Z, Mishal, J R, Jenkins, and E, May

Subjects

DNA-Binding Proteins, Transcriptional Activation, Dactinomycin, Tumor Cells, Cultured, Humans, Apoptosis, Cycloheximide, Tumor Suppressor Protein p53, Genes, p53, Transfection, Cell Division, HeLa Cells

Abstract

The p53 tumor suppressor gene has been implicated in the induction of apoptosis in several cell systems. We have recently reported than transiently-transfected wt p53 is capable of inducing apoptosis in certain transformed cell lines. We demonstrated by quantitative analysis using flow cytometry that apoptosis was restricted to the population expressing wt, but not mutant, p53. In the present study we use this model system to analyse the functional domain of p53 in the induction of apoptosis. Several constructs expressing mutations or deletions in the C-terminal oligomerization domain, the N-terminal transactivation domain or the central DNA-binding domain were introduced into HeLa cells, and the ability of the expressed proteins to induce apoptosis was evaluated. All the functional domains were found to be necessary for the induction of apoptosis. In addition, cycloheximide and actinomycin D inhibited wt p53-induced apoptosis. We therefore conclude that p53 acts in this cell system, at least in part, as a transcriptional activator in the induction of apoptosis.

Published

1995

6. Thioredoxin increases the proliferation of human B-cell lines through a protein kinase C-dependent mechanism

Author

C, Biguet, N, Wakasugi, Z, Mishal, A, Holmgren, S, Chouaib, T, Tursz, and H, Wakasugi

Subjects

Diglycerides, B-Lymphocytes, Thioredoxins, Escherichia coli, Tumor Cells, Cultured, Humans, Calcium, Inositol 1,4,5-Trisphosphate, Cell Division, Protein Kinase C, Signal Transduction

Abstract

Thioredoxin (Trx) catalyzes thiol-disulfide oxidoreductions. We and others recently showed that human Trx could function as an autocrine growth factor for human lymphoid cells immortalized by the human T-lymphotrophic virus type I or the Epstein-Barr virus. Here we report that reduced Trx from Escherichia coli generated by NADPH and thioredoxin reductase increases the proliferation of an Epstein-barr virus(+)-B cell line 1G8, which constitutively produces low amounts of human Trx. This proliferative effect involved the activation of protein kinase C through its translocation to the membrane. Staurosporin and calphostin C, two inhibitors of protein kinase C, but not of H8, a protein kinase A inhibitor, were able to block Trx-dependent proliferation. The addition of Trx to 1G8 cells resulted in the formation of inositol 1,4,5-triphosphate and sn-1,2-diacylglycerol by a phosphoinositide-specific phospholipase C, as well as increased free calcium concentration. Diacylglycerol showed a biphasic increase; the first phase, corresponding to an early peak (30 s) of inositol 1,4,5-triphosphate and a second larger, prolonged phase. The second phase was inhibited by propranolol, a specific inhibitor of phosphohydrolase, indicating that it is most likely derived from phosphatidylcholine hydrolysis by the sequential action of phospholipase D and phosphatidic acid phosphohydrolase. Our data suggest that enhanced phosphoinositide-specific phospholipase C activity induced by the dithiol form of Trx in 1G8 cells is associated to protein kinase C activation, and thus plays a role in the permanent growth of Epstein-Barr virus-infected B cells.

Published

1994

7. Induction of apoptosis by transiently transfected metabolically stable wt p53 in transformed cell lines

Author

E, Yonish-Rouach, J, Borde, M, Gotteland, Z, Mishal, A, Viron, and E, May

Abstract

Biochemical and functional properties of wild-type (wt) and mutant p53 were studied under the same cellular environment by transient transfection. Exogenous wt p53 expressed in transformed cell lines was found to be as metabolically stable as mutant p53. Yet only mutant p53 bound to hsp70 whereas wt p53 did not, suggesting that the metabolic stability of p53 does not depend on its ability to form complexes with hsp70. The wt protein was expressed essentially in the nucleus, while mutant p53 showed both nuclear and cytoplasmic expression, as determined by immunofluorescence staining with PAb122. In addition, staining with PAb1801 revealed a number of strongly fluorescent cell fragments in cultures transfected by wt p53. Morphological features of apoptosis were observed in these cultures. Quantitative analysis by flow cytometry confirmed that only the cell population expressing wt p53 had a significant amount of cell debris. Thus, transient expression of a metabolically stable wt, but not mutant, p53 induces cell death by apoptosis. The present study demonstrates a model system to investigate the functional domains of p53 in the induction of apoptosis.

Published

1994

8. Activation of an alpha-fetoprotein/receptor pathway in human normal and malignant peripheral blood mononuclear cells

Author

C, Esteban, J, Trojan, A, Macho, Z, Mishal, C, Lafarge-Frayssinet, and J, Uriel

Subjects

B-Lymphocytes, Receptors, Peptide, T-Lymphocytes, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Lymphocyte Activation, Burkitt Lymphoma, Immunohistochemistry, Monocytes, Leukocytes, Mononuclear, Tumor Cells, Cultured, Humans, Lymphoma, Large B-Cell, Diffuse, RNA, Messenger, alpha-Fetoproteins, In Situ Hybridization

Abstract

Alpha-fetoprotein (AFP) is mainly synthesized by the fetal liver and the yolk sac with minor contributions of several non-hepatic fetal tissues, variable according to the species considered. Most fetal cells, whatever their origin, possess the ability to bind and to endocytose the protein. This property, which is considered to be lost in differentiated cells of the adult, may be resumed in tumoral cells and is due to the expression of specific AFP receptors at the cell surface. Cytochemical and immunological approaches, combined with in situ hybridization, were used to investigate the specific uptake and synthesis of human AFP in several classes of peripheral blood mononuclear cells (PBMC) and in several malignant cell lines of hematopoietic origin. With the exception of quiescent T lymphocytes, all cells investigated specifically bound AFP. Both normal and malignant blood mononuclear cells expressed mRNA transcripts of AFP which were translated into the protein during a well established period of cellular growth. These results suggest that an AFP/receptor autocrine system might operate in normal and malignant blood mononuclear cells. Its physiological role is discussed in relation to recent work from our laboratory--providing experimental evidence that AFP, throughout its interaction with specific cell receptors, regulates and facilitates the entry of fatty acids into living cells undergoing growth and differentiation.

Published

1993

9. Receptor-mediated uptake and processing of vitamin D-binding protein in human B-lymphoid cells

Author

C, Esteban, M, Geuskens, J M, Ena, Z, Mishal, A, Macho, J M, Torres, and J, Uriel

Subjects

Organelles, B-Lymphocytes, Vitamin D-Binding Protein, Biological Transport, Receptors, Cell Surface, Binding, Competitive, Burkitt Lymphoma, Cell Line, Iodine Radioisotopes, Kinetics, Multigene Family, Animals, Humans, Cattle, alpha-Fetoproteins, Horseradish Peroxidase, Serum Albumin

Abstract

Vitamin D-binding protein (DBP), a member of a multigene family including alpha-fetoprotein (AFP) and albumin, is a serum glycoprotein that reversibly binds and transports vitamin D and its metabolites to target cells. In this work, we demonstrate that normal and malignant human B-lymphocytes specifically bind and internalize DBP. Radioiodinated DBP (125I-DBP) was used to follow the uptake of the protein by Raji cells, a human pre-B-lymphoma cell line. Time course studies of DBP uptake by these cells exhibited a saturable profile at both 4 and 37 degrees C. The binding saturation curve obtained by incubating Raji cells at 4 degrees C with different concentrations (1.5 nM to 1.5 microM) of 125I-DBP showed two saturation plateaus; Scatchard analysis showed the presence of two groups of receptor sites with a Kd1 of 2.04 x 10(-7) M (n1 = 42,161 +/- 4,336 sites/cell) and a Kd2 of 1.01 x 10(-6) M (n2 = 198,000 +/- 48,000 sites/cell). After incubation of Raji cells at 37 degrees C with both fluorescein isothiocyanate (FITC) and horseradish peroxidase conjugates, DBP was internalized and could be localized in the cytoplasm. DBP-horseradish peroxidase conjugates were used to follow the uptake and to determine the endocytic pathway of the protein in Raji cells. The initial steps, contrary to those observed for AFP, did not apparently involve coated pits and vesicles. Small vesicles (approximately 50-60 nm) with electron-dense DBP-horseradish peroxidase reaction products were observed that could fuse with large endosomes. These endosomes appeared dispersed in the cytoplasm with some preferential localization in the Golgi centrosphere region. Pulse-chase experiments showed that only 10% of the uptaken protein was released in a nondegraded form. Accordingly, most DBP molecules accumulated in endosomes should be degraded in lysosomes, instead of being recycled back to the surface, as in the case of AFP. Contrary to malignant B-cells (Raji), the uptake ability for DBP of normal quiescent B-lymphocytes was very low. Specific binding and internalization of DBP-FITC by these cells were observed following mitogen-induced activation. Significant values of uptake were obtained at 37 degrees C after 72 h of incubation in the presence of pokeweed mitogen. The binding of DBP-FITC was partially inhibited in the presence of an excess of unlabeled protein. Taken together, the actual results suggest that DBP receptors are constitutively expressed by malignant B-cells and in a transitory form by normal B-lymphocytes undergoing mitogen-induced activation.(ABSTRACT TRUNCATED AT 400 WORDS)

Published

1992

10. Abnormally expanded CD8+/Leu-7+ lymphocytes persisting in long-term bone marrow-transplanted patients are resting pre-cytotoxic T-lymphocytes

Author

E, Leroy, L, Madariaga, M, Ben Aribia, Z, Mishal, I, Theodorou, H, Rochant, J P, Vernant, and A, Senik

Subjects

Antigens, Differentiation, T-Lymphocyte, Cytotoxicity, Immunologic, CD8 Antigens, T-Lymphocytes, Cell Differentiation, Cell Separation, Lymphocyte Activation, Antigens, Differentiation, CD57 Antigens, Pokeweed Mitogens, Antigens, CD, Humans, Bone Marrow Transplantation, T-Lymphocytes, Cytotoxic

Abstract

We analyzed the functional status of the small CD8+/Leu-7+ T-lymphocytes that circulate in increased proportions in the blood of many allogeneic bone marrow transplant (BMT) patients. Purified CD8+/Leu-7+ T cells were tested for their effect on T-cell proliferative responses. In contrast to CD8+/Leu-7-T-lymphocytes, such cells behaved as suppressor cells for lectin-induced mitogenic responses of the donor's peripheral blood lymphocytes. However, they did not interfere with the in vitro responsiveness to specific stimuli such as protein purified derivative (PPD) or alloantigens. We demonstrate that CD8+/Leu-7+ T cells are resting pre-cytotoxic T-lymphocytes (CTL) that can be induced by mitogenic lectins to express their cytolytic program in a non-specific, non-major histocompatibility complex-restricted manner against phytohemagglutinin-treated lymphoblasts or K562 target cells. The lectin-triggered cytotoxicity was achieved within a few days, together with limited cell division. Our results suggest that circulating CD8+/Leu-7+ T cells from BMT recipients are in vivo primed CTL awaiting cellular activation.

Published

1990

11. Interleukin-4 induces selection of human penicillin-specific CD4+ lymphocytes through regulation of cell cycle G1/S transition and apoptosis

Author

I. Gaspard, A. Vervisch, Z. Mishal, Hervé Lebrec, and Marc Pallardy

Subjects

S-phase-promoting factor, G1/S transition, General Medicine, Cell cycle, Biology, Toxicology, Cell biology, Penicillin, Apoptosis, medicine, Restriction point, Interleukin 4, Selection (genetic algorithm), medicine.drug

Published

1998

12. A method for the quantitative detection of human acute lymphatic leukemia

Author

Michael Inbar, N. Larnicol, C. Rosenfeld, Augery Y, Mathé G, Claude Jasmin, and Z. Mishal

Subjects

Pathology, medicine.medical_specialty, Viscosity, Membrane lipids, Lymphocyte, General Medicine, Biology, Prognosis, medicine.disease, Fluorescence, Molecular biology, Leukemia, Lymphoid, Microviscosity, Membrane Lipids, Leukemia, Spectrometry, Fluorescence, Membrane, medicine.anatomical_structure, medicine, Humans, Lymphocytes, Lipid bilayer, Fluorescence anisotropy

Abstract

Lymphocytes isolated from the peripheral blood of 32 patients with acute lymphatic leukemia (ALL), 4 patients with non-leukemia malignant disorders and from 12 normal healthy donors were studied for fluidity of membrane lipids. The degree of fluidity of cellular membranes was determined by fluorescence polarization analysis using the fluorescent probe 1,6-diphenyl 1,3,5-hexatriene (DPH), when embedded in membrane lipid region of intact cells. Based on the fluorescence polarization (P) analysis the degree of membrane microviscosity ( \ gh) was determined. Results have shown that lymphocytes isolated from untreated ALL patients have a more fluid lipid layer in their cellular membrane (average of 17 patients \ gh = 2.65 poise at 25°C) than lymphocytes isolated from normal donors (average of 12 donors \ gh = 3.91 poise at 25°C). The results also showed that the degree of membrane lipid microviscosity of lymphocytes isolated from ALL patients in partial or complete clinical remission is similar to that of normal lymphocyte (average of 15 patients \ gh = 3.89 poise at 25°C). Lymphocytes isolated from patients with non-leukemic malignant disorders showed a similar characteristic to normal lymphocytes. These results which confirmed our previous observations with other leukemias are in line with the suggestion that fluorescence polarization analysis of DPH labelled lymphocytes can serve as a quantitative clinical tool for human acute lymphatic leukemia.

Published

1977

13. Quantification of oestradiol binding at the surface of human lymphocytes by flow cytofluorimetry

Author

P.M. Martin, Y. Berthoix, F. Le Caer, N. Tubiana, J M Seigneurin, Y Carcassonne, and Z. Mishal

Subjects

endocrine system, Cancer Research, B-Lymphocytes, Estradiol, Chemistry, T-Lymphocytes, Cell Separation, Receptors, Estradiol, In Vitro Techniques, Flow Cytometry, Oncology, Flow (mathematics), Immunology, polycyclic compounds, Biophysics, Humans, Lymphocytes, skin and connective tissue diseases, hormones, hormone substitutes, and hormone antagonists, Research Article

Abstract

Quantification of oestradiol binding at the surface of human lymphocytes by flow cytofluorimetry

Published

1986

14. Transformation of LMTK- cells with purified class I genes. V. Antibody-induced structural modification of HLA class I molecules results in potentiation of the fixation of a second monoclonal antibody

Author

F A Lemonnier, P P Le Bouteiller, D Olive, B Malissen, Z Mishal, C Layet, J Dubreuil, D H Caillol, F M Kourilsky, and B R Jordan

Subjects

Immunology, Immunology and Allergy

Abstract

A potentiation phenomenon was observed with HLA-A3 and CW3 transformed murine L cells between anti-HLA class I B10.6 (potentiated) and B10.8 (potentiating) monoclonal antibodies (m.Ab.). Further studies of this phenomenon with these transformed L cells indicated that: 1) no significant specific binding of B10.6 m.Ab. to HLA-A3 and CW3 transformed L cells could be demonstrated by conventional radioimmunoassay or cytofluorometric study in the absence of B10.8 m.Ab.; 2) potentiation of the fixation of B10.6 m.Ab. was induced by other anti-HLA class I m.Ab., which all reacted with the same cluster of antigenic determinants; 3) potentiation reflects an increased specific fixation of B10.6 m.Ab. to HLA class I molecules implicating its combining site; 4) potentiation was mediated by B10.8 Fab fragments. These results indicate that potentiation of the fixation of B10.6 m.Ab. to the HLA-A3 and CW3 molecules expressed by the transformed L cells reflects conformational changes of these molecules after interaction with B10.8 m.Ab.

Published

1984

15. Decreased microviscosity of membrane lipids in leukemic cells: Two possible mechanisms

Author

M. Petitou, M. Paintrand, Françoise Phan Dinh Tuy, G. Mathe, C. Rosenfeld, C. Jasnin, Michael Inbar, and Z. Mishal

Subjects

Cellular membrane, Optical Rotation, Lipoproteins, Membrane lipids, Cell, Cell membrane, Microviscosity, Membrane Lipids, Blood serum, medicine, Humans, Lymphocytes, Biological Sciences: Cell Biology, Multidisciplinary, Viscosity, Chemistry, Cell Membrane, Molecular biology, Leukemia, Lymphoid, Pleural Effusion, Spectrometry, Fluorescence, Membrane, medicine.anatomical_structure, Biochemistry, lipids (amino acids, peptides, and proteins), Fluorescence anisotropy

Abstract

Steady-state fluorescence polarization studies with the fluorescent lipid probe 1,6-diphenyl 1,3,5-hexatriene were done to determine the degree of microviscosity of cellular membrane lipids and serum lipoproteins in human normal donors and leukemic patients. The results show a marked decrease in microviscosity of cellular membrane lipids in both intact lymphocytes and isolated cellular plasma membranes obtained from leukemic patients in clinical relapse as compared to intact lymphocytes and isolated cellular plasma membranes obtained from normal donors and leukemic patients in complete clinical remission. Concomitant to these dynamic changes in cellular membrane lipids, the degree of microviscosity of lipids in the blood serum of leukemic patients in clinical relapse is markedly reduced as compared to serum obtained from normal donors and leukemic patients in complete clinical remission. Moreover, an in vitro incubation of leukemic lymphocytes with normal low density lipoproteins results in an increased microviscosity of cellular membrane lipids. In addition to the interrelation between cellular membrane lipids and serum lipoproteins, plasma membrane vesicles with a high degree of lipid microviscosity were isolated from the blood serum and pleural effusion of leukemic patients in clinical relapse. Such membrane vesicles could not be detected in normal serum. Therefore, we suggest that the two major mechanisms associated with the decreased microviscosity of membrane lipids in human leukemic cells are an abnormal exchange in lipids between the leukemic cell surface membrane and leukemic serum lipoproteins and an exfoliation of plasma membrane vesicles with a high degree of microviscosity from the cell surface of leukemic cells.

Published

1978

16. Correction by insulin added in vitro of abnormal membrane fluidity of the erythrocytes from Type 1 (insulin-dependent) diabetic patients

Author

Z. Mishal, M. F. Aillaud, C. Roul, Y. Mourayre, Irène Juhan-Vague, D. Rahmani-Jourdheuil, and Philippe Vague

Subjects

Adult, Male, medicine.medical_specialty, Membrane Fluidity, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Fluorescence Polarization, In Vitro Techniques, Biology, In vivo, Diabetes mellitus, Internal medicine, Internal Medicine, medicine, Membrane fluidity, Humans, Insulin, Lipid bilayer, Red Cell, Erythrocyte Membrane, Middle Aged, medicine.disease, Red blood cell, Diabetes Mellitus, Type 1, medicine.anatomical_structure, Endocrinology, Female, Fluorescence anisotropy, Proinsulin

Abstract

Filtrability of erythrocytes obtained from uncontrolled Type 1 (insulin-dependent) diabetic patients is abnormal, but is corrected by insulin added in vivo or in vitro. As erythrocyte filtrability depends on several determinants, we chose to study a membrane property of erythrocytes from diabetic subjects. Membrane fluidity was studied by fluorescence polarization using a lipophilic probe, the diphenyl-hexatriene and the Coulter Epics V together with a laser Spectra-physics 2000. Fluorescence polarization values obtained for 31 normal subjects (0.253 +/- 0.043 SD) and 31 uncontrolled Type 1 diabetic patients (0.231 +/- 0.043 SD) were significantly different (p less than 0.01). Insulin (2.5.10(-9) mol/l) added in vitro increased the fluorescence polarization values of red cell membranes from diabetic patients (without insulin, fluorescence polarization values = 0.210 +/- 0.032 SD; with insulin, fluorescence polarization values = 0.253 +/- 0.024 SD, p less than 0.001, n = 15), but had no effect on normal membranes (without insulin fluorescence polarization values = 0.255 +/- 0.037 SD, with insulin, fluorescence polarization values = 0.251 +/- 0.026 SD; n = 12). Given a relationship between the lipid bilayer and membrane cytoskeleton proteins, this insulin-correctable abnormality of erythrocyte membrane fluidity may be an important determinant of the rheological behaviour of erythrocytes from diabetic patients.

Published

1986

17. The effect of hexamethylene-bis-acetamide on multiparameter analysis of friend leukemia cells

Author

H. Tapiero, A. Fourcade, and Z. Mishal

Subjects

Friend leukemia, Biophysics, Cell Separation, Diamines, Dexamethasone, Cell Line, Pathology and Forensic Medicine, Mice, chemistry.chemical_compound, Endocrinology, Acetamides, medicine, Animals, Distribution (pharmacology), Erythropoiesis, Leukemia, Experimental, Chemistry, Cell growth, Cell Membrane, Cell Differentiation, Cell Biology, Hematology, Flow Cytometry, Fluorescence, Friend murine leukemia virus, Fluorescence activated cell sorter, Immunology, Diphenylhexatriene, Fluorescence anisotropy, Acetamide, medicine.drug

Abstract

Friend leukemia cells were induced to differentiate by hexamethylene-bis-acetamide (HMBA). The relationship between cell growth cell volume distribution, fluorescence intensity and fluorescence anisotropy of the membrane probe 1,6 diphenyl 1,3,5 hexatriene (DPH) was analyzed in differentiated and undifferentiated cells with the aid of the fluorescence activated cell sorter (FACS II). The induction of a differentiated state was associated with a decrease in cell volume and an increase of fluorescence anisotrophy. The inhibition of this induction by dexamethasone prevented the decrease of cell volume without affecting the increase of fluorescence anisotropy. We conclude therefore that the high degree of anisotropy is not correlated to the differentiated state nor with the volume of the cells.

Published

1981

18. Transformation of murine LMTK- cells with purified HLA class I genes. I. Modification of conformation of murine beta 2-microglobulin upon its association with HLA heavy chains

Author

F A Lemonnier, P P Le Bouteiller, B Malissen, P Golstein, M Malissen, Z Mishal, D H Caillol, B R Jordan, and F M Kourilsky

Subjects

Immunology, Immunology and Allergy

Abstract

Murine LMTK- cells were unexpectedly found to cross-react with a murine anti-human beta 2-microglobulin (beta 2-m)monoclonal antibody (m.Ab) after transformation with cosmid clones containing different purified HLA class I genes. The same cross-reactivity was observed with CTP 34 B4 (murine x human) somatic hybrid cells, which express class I molecules constituted of human HLA heavy chains and murine beta 2-m. Inhibition studies of the complement-dependent cytolysis mediated by the cross-reacting m.Ab indicated that isolated murine beta 2-m does not express the cross-reacting determinant, suggesting that its expression by the transformed cells reflects conformational modification of murine beta 2-m upon its association with HLA heavy chains. These results illustrate one of the possible post-translational mechanisms through which the antigenicity of a polypeptide chain can be modified. They might provide a serologic marker of the third domain of HLA class I heavy chains. Finally, because quantitative differences of reactivity with the anti-human beta 2-m m.Ab were observed, depending on the HLA class I genes used for transformation, these results individualize two families of HLA class I heavy chains responsible for different conformational modifications of murine beta 2-m.

Published

1983

19. Persistence of T8+/HNK-1+ suppressor lymphocytes in the blood of long-term surviving patients after allogeneic bone marrow transplantation

Author

E Leroy, C F Calvo, M Divine, M F Gourdin, F Baujean, M H Ben Aribia, Z Mishal, J P Vernant, J P Farcet, and A Senik

Subjects

Immunology, Immunology and Allergy

Abstract

Fifteen patients and their respective bone marrow donors were entered in this study 1 to 5 yr after allogeneic bone marrow transplantation. Peripheral blood E rosetting (T) cells were analyzed for their phenotypic characteristics as well as for their ability to regulate Ig synthesis in the in vitro PWM system. A close relationship was found between a high proportion of T8+/HNK-1+ cells and/or T8+/HLA-DR+ cells and a strong (greater than or equal to 50%) inhibition of the antibody response. It was noteworthy that even the patients without suppressor activity had high proportions of such cells when compared with normal marrow donors. Moreover, the suppression occurred irrespective of the presence or absence of chronic GVHD. Through negative selection experiments (with MAb and complement) and through immunofluorescence cell sorting, it was shown that the suppressor cells expressed the T8+, HNK-1+, HLA-DR- phenotype. They did not carry the Leu-11, NKH1A, or NKH2 determinants, which are expressed on mature functional NK cells. When examined by electron microscopy, they exhibited a morphology of resting agranular lymphocytes. The significant increase of these suppressor cells among the BMT patients was not correlated with clinical syndromes such as chronic GVHD or opportunistic viral infections, which argues against the notion of in vivo profound immunodeficiency coexisting with these cells.

Published

1986

20. Altered lipid microviscosity in lymphoblastoid cells treated with 12-O-tetradecanoyl phorbol 13-acetate, a tumor promoter

Author

C. Rosenfeld, C. Rochette-Egly, M. Castagna, and Z. Mishal

Subjects

Biophysics, Biochemistry, 12 o tetradecanoyl phorbol 13 acetate, Cell Line, Microviscosity, Mice, Structural Biology, Genetics, Animals, Humans, Lymphocytes, Leukemia L1210, Molecular Biology, Cells, Cultured, Phospholipids, Leukemia, Chemistry, Viscosity, Lymphoblast, Cell Biology, Lipid Metabolism, Phorbols, Kinetics, Cholesterol, Spectrometry, Fluorescence, Liposomes, Tetradecanoylphorbol Acetate

21. Correction by pentoxifylline of the abnormal fluorescence polarization of erythrocyte membranes from diabetic patients

Author

Z. Mishal, J. Le Petit, C. Roul, P. Vague, Y. Mourayre, D. Rahmani-Jourdheuil, and I. Juhan-Vague

Subjects

Adult, medicine.medical_specialty, Membrane lipids, Fluorescence Polarization, Pentoxifylline, Internal medicine, Diabetes mellitus, medicine, Membrane fluidity, Humans, Pharmacology (medical), Pharmacology, Chemistry, Erythrocyte Membrane, General Medicine, Middle Aged, medicine.disease, Red blood cell, Membrane, Endocrinology, medicine.anatomical_structure, Diabetes Mellitus, Type 1, Mechanism of action, Theobromine, medicine.symptom, Fluorescence anisotropy, medicine.drug

Abstract

Erythrocytes from diabetic patients show abnormal rheology. Pentoxifylline, a methylxanthine, improves the abnormal deformability of diabetic erythrocytes, but its mechanism of action remains unclear. We have studied the effect of pentoxifylline on the lipid order of erythrocyte membranes from controls and patients with Type I diabetes. We studied the structural organization of membrane lipids in individual erythrocyte ghosts by fluorescence polarization using a cell sorter. Fluorescence polarization values (P) for 17 controls (P = 0.244) and 20 diabetic patients (P = 0.215) were significantly different. Pentoxifylline added in vitro had no effect on normal membranes, but significantly increased at 10(-5) mol X l-1 (P = 0.233), and normalized at 10(-4) mol X l-1 (P = 0.243), the P value of membrane ghosts from diabetics.

Published

1987

22. Expression and Characterization of Leucocyte Antigens

Author

R. Allen, S. Ferrone, J. Hoch, A. Bankhurst, J. Spellmann, G. R. Burmester, A. Dimitriu-Bona, P. Gregersen, S. J. Waters, R. J. Winchester, O. R. Burrone, F. Calabi, D. Gilmore, B. Wright, C. Milstein, E. Clark, P. Martin, J. Hansen, J. Ledbetter, L. de Leij, S. Poppema, T. H. The, J. E. De Vries, R. Vaessen, P. Janssens, B. Tan, A. Heiman, C. G. Figdor, B. Dörken, M. Pfreundschuh, G. Moldenhauer, E. Schwarz, G. Hämmerling, D. Frisman, S. Baird, E. Gazit, Y. Gothelf, R. Gil, S. Orgad, E. J. Yunis, Ch. Girardet, D. Heumann, J.-P. Mach, V. von Fliedner, S. Carrel, S. M. Goyert, J. Silver, N. Hogg, P. Hokland, S. F. Schlossman, J. Ritz, J. Kalil, J. P. Abita, C. Chomienne, O. Poirier, D. Besluau, H. Dastot, M. Reboul, M. Fellous, J. Colombani, L. Kater, P. Brekelmans, T. Daemen, H. J. Schuurman, F. Katz, S. Povey, K. Stanley, C. Schneider, M. Greaves, F. A. Lemonnier, P. P. Le Bouteiller, B. Malissen, P. Golstein, M. Malissen, Z. Mishal, D. H. Caillol, B. R. Jordan, F. Kourilsky, K. Lennert, H. Stein, H. K. Miiller-Hermelink, R. Vollenweider, R. A. Karol, J. Eng, D. Dennison, E. Faris, D. M. Marcus, D. Piatier-Tonneau, B. Boyer, P. Debre, D. Charron, J. M. Reuben, E. M. Hersh, P. W. A. Mansell, G. Newell, A. Rios, H. Rumpold, D. Kraft, O. Förster, T. F. Schulz, J. Alsenz, O. Scheiner, J. Lambris, M. P. Dierich, J. P. R. M. Van Laarhoven, R. Broekhuizen, G. Th. Spierenburg, C. H. M. M. De Bruyn, W. Solbach, M. Röllinghoff, H. Wagner, I. S. Szer, A. Irani, W. J. M. Tax, G. Janossy, M. Jonker, R. Willems, J. Leeuwenberg, P. J. A. Capel, R. A. P. Koene, H. F. M. Leeuwenberg, H. M. Willems, P. A. T. Tetteroo, F. Visser, P. Landsdorp, A. E. G. Kr. von dem Borne, J. S. Thompson, N. E. Goeken, S. A. Brown, J. R. Rhoades, K. Yamamoto, H. Nakauchi, H. Karasuyama, K. Kitamura, K. Tanimoto, and K. Okumura

Subjects

Antiserum, Gel electrophoresis, Messenger RNA, Antigen, Immunoprecipitation, Chemistry, Translation (biology), Pan-T antigens, Molecular biology, Raji cell

Abstract

In vitro translation and immunoprecipitation were used to identify messenger RNAs (mRNAs) coding for lymphocyte surface antigens. The mRNAs were extracted from human lymphoblastoid cell lines of B-cell or T-cell origin. Messenger RNA was also extracted from fibroblastoid lines as non-lymphoid control. Translation products were reacted with a xenoantiserum raised against human lymphoid surface antigens. Products immunoprecipitated with antiserum were analyzed by SDS-polyacrylamide gel electrophoresis and fluorography.

Published

1984

23. Expression of platelet glycoprotein Ib alpha in HEL cells

Author

N, Kieffer, N, Debili, A, Wicki, M, Titeux, A, Henri, Z, Mishal, J, Breton-Gorius, W, Vainchenker, and K J, Clemetson

Subjects

Blood Platelets, Molecular Weight, Platelet Glycoprotein GPIb-IX Complex, Tunicamycin, Asialoglycoproteins, Humans, Oligosaccharides, Leukemia, Erythroblastic, Acute, Platelet Membrane Glycoproteins, Cell Line

Abstract

We have previously shown that platelet glycoprotein Ib is expressed in a minority of cells of the human leukemic cell line HEL (Tabilio, A., Rosa, J. P., Testa, U., Kieffer, N., Nurden, A. T., Del Canizo, M. C., Breton-Gorius, J., and Vainchenker, W. (1984) EMBO J. 3, 453-459). In this report, we have selected a stable HEL subclone with increased expression of glycoprotein (GP) Ib as assessed by 6 different monoclonal antibodies in order to investigate the biochemical characteristics of this glycoprotein. A single polypeptide chain of apparent Mr = 60,000 was precipitated under reducing and nonreducing conditions by a specific polyclonal anti-platelet glycocalicin antibody and two anti-GPIb alpha monoclonal antibodies (AN51 and AP1), both from surface-labeled and metabolically labeled HEL cells. We were unable to demonstrate the presence of a polypeptide corresponding to the beta subunit of GPIb or GPIX which is closely associated with GPIb. Competitive immunoprecipitation performed in the presence of an excess amount of cold platelet glycocalicin completely displaced the Mr = 60,000 polypeptide. Synthesis of N-linked oligosaccharide chains on this Mr = 60,000 polypeptide was inhibited by the antibiotic tunicamycin, and a shift of the apparent Mr from 60,000 to 48,000 was observed. O-Linked oligosaccharide chains identical to platelet GPIb hexasaccharides were deficient or incomplete since no peanut agglutinin binding to the Mr = 60,000 polypeptide was observed after neuraminidase treatment of HEL cells. Thus, our results provide evidence that the Mr = 60,000 polypeptide expressed on the surface membrane of HEL cells is closely related to platelet GPIb and corresponds to an incompletely or abnormally O-glycosylated GPIb alpha subunit.

Published

1986

24. Changes in biophysical parameters and in phospholipid composition associated with resistance to doxorubicin

Author

H, Tapiero, Z, Mishal, M, Wioland, A, Silber, A, Fourcade, and G, Zwingelstein

Subjects

Electrophoresis, Leukemia, Experimental, Doxorubicin, Drug Resistance, Fluorescence Polarization, Cells, Cultured, Phospholipids, Friend murine leukemia virus

Abstract

Friend leukemia cells (FLC) resistant to different concentrations of doxorubicin were used to investigate the biochemical and biophysical changes associated with resistance. We have found that fluorescence polarization of 1,6-diphenyl-1,3,5-hexatriene analyzed on single cell level increased in resistant as compared to sensitive FLC. Furthermore, phospholipid analysis of sensitive and doxorubicin-resistant cells revealed changes in ratios of phosphatidyl-choline to phosphatidyl-ethanolamine and phosphatidyl-choline to sphingomyelin. These results correlate with decreased electrophoretic mobility in resistant cells. Our results indicate that changes in cell structure occur with the level of resistance to doxorubicin. These changes are probably the consequence rather than the cause of resistance.

Published

1986

25. Supernatant from a cloned helper T cell stimulates most small resting B cells to undergo increased I-A expression, blastogenesis, and progression through cell cycle

Author

L, Leclercq, J C, Cambier, Z, Mishal, M H, Julius, and J, Theze

Subjects

B-Lymphocytes, Lymphokines, Staining and Labeling, Cell Cycle, Histocompatibility Antigens Class II, Immunoglobulins, Cell Differentiation, T-Lymphocytes, Helper-Inducer, Flow Cytometry, Lymphocyte Activation, Acridine Orange, Clone Cells, Culture Media, Mice, Inbred C57BL, Mice, Mice, Inbred DBA, Animals, Interleukin-4, Growth Substances, Interphase

Abstract

Helper T cell clone 52.3 supernatant (52.3 SN) was previously shown to be able to stimulate gradient-purified murine resting B cells in the absence of any additional stimulus. However, the proportion of cells that were accounting for the thymidine uptake and the Ig production was unknown. In this paper, we have studied induced changes that can be measured at the single cell level, and have thus determined the frequency of resting B cells that respond to 52.3 SN. Results indicate that 52.3 SN induces an increased I-A expression and a cell size enlargement on virtually all resting B cells. A significant proportion (30%) of these cells later becomes large blasts. Acridine orange staining revealed that in the presence of 52.3 SN a large fraction of the resting B cells undergoes the G0 to G1 transition. Furthermore, 52.3 SN is able to induce at least 20% of the cells to continue through the cell cycle into S phase as indicated by propidium iodide staining of DNA. Finally, a fraction of the 52.3 SN-stimulated cells differentiate to Ig-producing cells. Our present results suggest that resting B cells express functional receptors for some lymphokines and that these lymphokines can act in the absence of membrane Ig occupancy. Our findings further support the existence of a B cell-activating factor acting in a MHC-unrestricted manner and responsible for the entry of resting B cells into cell cycle. The relationship between this factor and other lymphokines is discussed.

Published

1986

26. Rapid modifications of biophysical and biochemical parameters of red blood cell membrane from insulin dependent diabetics after insulin administration

Author

I, Juhan-Vague, C, Roul, D, Rahmani-Jourdheil, Z, Mishal, F, Driss, M, Durand-Gasselin, M F, Aillaud, and P, Vague

Subjects

Membrane Lipids, Diabetes Mellitus, Type 1, Erythrocyte Deformability, Erythrocyte Membrane, Humans, Insulin, Ca(2+) Mg(2+)-ATPase, Sodium-Potassium-Exchanging ATPase, Rheology

Abstract

We have previously shown that red blood cell (RBC) filtrability in uncontrolled insulin dependent diabetics is abnormal compared to healthy subjects, but is corrected by insulin added in vivo or in vitro. We have now found biophysical abnormalities of the RBC membrane in such patients: Fluorescence polarization value (p) evaluated using DPH as probe is significantly lower in patients; insulin added in vitro increases and normalises the p value of diabetic RBC membrane, and has no effect on normal RBC membrane. As there is a relationship between the lipid bilayer and membrane cytoskeleton proteins, this abnormality of RBC membrane fluidity, correctable by insulin, may be an important determinant of the rheological behaviour of the RBC. In parallel, biochemical abnormalities of the RBC membrane are shown in the same patients: Higher cholesterol/phospholipid ratio, lower content in unsaturated fatty acids and higher content in saturated fatty acids. Decreased activity of ouabaine sensitive Na+K+ ATPase and increased activity of Mg++ ATPase. All of these RBC biochemical abnormalities are corrected after 24 h of normoglycaemia obtained by insulin treatment given in vivo with a biostator. Our results show the importance to check the degree of control of glycaemia when studying rheological parameters in diabetes mellitus.

Published

1986

27. Reactivity of the Anti-Human T Cell Monoclonal Antibodies Submitted to the Workshop on One Anti-Class I and One Anti Class II Cytotoxic T Cell Clone

Author

B. Malissen, D. Olive, N. Rebai, Z. Mishal, and C. Mawas

Subjects

medicine.anatomical_structure, medicine.drug_class, Chemistry, T cell, Immunology, medicine, Cytotoxic T cell, Clone (B-cell biology), Monoclonal antibody, Molecular biology

Abstract

The monoclonal antibodies (mAbs) submitted to the T cell protocol were screened on two stable cytotoxic clones previously obtained in this laboratory [1, 5].

Published

1984

28. [The effect of pentoxifylline and propentofylline on the membrane fluidity of red blood cells in uncontrolled insulin-dependent (type 1) diabetic patients]

Author

C, Roul, I, Juhan-Vague, D, Rahmani-Jourdheuil, Z, Mishal, and P, Vague

Subjects

Diabetes Mellitus, Type 1, Membrane Fluidity, Xanthines, Erythrocyte Membrane, Humans, Theobromine, Fluorescence Polarization, Pentoxifylline, Diphenylhexatriene

Abstract

Fluorescence polarization of red blood cell (RBC) membranes evaluated using DPH was measured in patients with uncontrolled insulin-dependent diabetes mellitus and in controls. The effect of in vitro addition of pentoxifylline and propentofylline (10(-5) and 10(-4) M) was studied. The fluorescence polarization parameter (P) was lower in the diabetic patients (p = 0.20 +/- 0.03, n = 8) as compared to the controls (p = 0.28 +/- 0.02), n = 8), reflecting an increase in probe mobility in the hydrophobic environment in the depth of the double lipid layer. In vitro addition of pentoxifylline had no effect on the fluorescence parameter of RBC membranes from controls, whereas both concentrations of pentoxifylline studied (p = 0.24 +/- 0.03) significantly increased the fluorescence parameter of RBC membranes from diabetics. Propentofylline had no effect. These findings suggest that the active site responsible for improved membrane fluidity of RBC from diabetics is located on the methyl radical present in the pentoxifylline molecule but not in the propentofylline molecule.

Published

1988

29. Endocytosis of HLA and H-2 molecules on transformed murine cells measured by fluorescence dequenching of liposome-encapsulated carboxyfluorescein

Author

Z. Mishal, F. A. Lemonnier, Jacques Barbet, Patrick Machy, L. D. Leserman, and A. Truneh

Subjects

media_common.quotation_subject, education, Fluorescence spectrometry, Human leukocyte antigen, Simian virus 40, Biology, Major histocompatibility complex, Endocytosis, General Biochemistry, Genetics and Molecular Biology, Major Histocompatibility Complex, Epitopes, Mice, L Cells, Antigen, HLA Antigens, Animals, Humans, Internalization, Molecular Biology, media_common, Liposome, General Immunology and Microbiology, General Neuroscience, H-2 Antigens, Antibodies, Monoclonal, Cell Transformation, Viral, Fluoresceins, Molecular biology, Cell biology, Histocompatibility, Methotrexate, Spectrometry, Fluorescence, Liposomes, biology.protein, Research Article, HeLa Cells

Abstract

We have studied internalization of cell surface proteins encoded by genes of the human major histocompatibility complex (HLA) transferred into murine L cells, in comparison with mouse (H-2) histocompatibility determinants. This internalization was measured by the use of monoclonal antibodies directed at these determinants, to which were bound methotrexate- and carboxyfluorescein-containing liposomes covalently coupled to protein A. In addition to the effect of methotrexate on the cells, the technique of fluorescence self-quenching release was used to measure the kinetics of internalization for single cells using a flow cytofluorometer. The native and foreign gene products were internalized in an apparently identical manner. These techniques can be applied to cells expressing genes with altered or deleted segments thus providing a basis for the analysis of the effect of sequence modifications on the internalization of the encoded molecule.

Published

1983

30. Effect of pH on fluorescence polarization of DMSO induced Friend leukemic cells

Author

Z, Mishal, F, Tuy, C, Billard, and H, Tapiero

Subjects

Membrane Lipids, Leukemia, Experimental, Membrane Fluidity, Cell Membrane, Animals, Membrane Proteins, Dimethyl Sulfoxide, Fluorescence Polarization, Hydrogen-Ion Concentration, Diphenylhexatriene, Cells, Cultured, Friend murine leukemia virus

Abstract

The effect of DMSO on Friend leukemic cell membranes was investigated in an inducible cell line (FLC) and in cell variant resistant to DMSO induction (RFLC). Fluorescence polarization (P) studies carried out at 37 degrees C with diphenyl hexatriene (DPH) have shown that P values change according to the pH, being maximum in alkaline buffer. These changes were altered when cells were grown in the presence of DMSO. Changes in P values according to the pH were abolished by glutaraldehyde and by sodium azide. Fluorescence polarization analysis of FLC cell line carried out at 4 degrees C have shown higher P values which also changed according to the pH. In DMSO induced FLC or in RFLC grown with or without DMSO, these changes were not seen. It is therefore concluded that P value changes related to pH reflect changes in the lipid-protein interactions of cell surface membrane. It is also suggested that these interactions are altered by DMSO.

Published

1981

31. Expression of platelet proteins during maturation of human megakaryocytes and of the K 562/HEL cell lines

Author

W, Vainchenker, N, Kieffer, E, Cramer, G, Vinci, N, Debili, A, Henri, M, Titeux, J, Guichard, Z, Mishal, and J, Breton-Gorius

Subjects

Blood Platelets, Phenotype, Humans, Blood Proteins, Platelet Membrane Glycoproteins, Cytoplasmic Granules, Hematopoietic Stem Cells, Megakaryocytes, Cell Line, Glycoproteins, Hematopoiesis

Published

1986

32. HLA class-I and class-II antigen expression by human leukemic K562 cells and by Burkitt-K562 hybrids: modulation by differentiation inducers and interferon

Author

D, Garson, M C, Dokhélar, H, Wakasugi, Z, Mishal, and T, Tursz

Subjects

Leukemia, Cell Differentiation, Hybrid Cells, Burkitt Lymphoma, Cell Line, Butyrates, Interferon-gamma, Phenotype, Gene Expression Regulation, HLA Antigens, Interferon Type I, Butyric Acid, Humans, Tetradecanoylphorbol Acetate, Lyngbya Toxins

Abstract

K562 cells, which could be regarded as pluripotent hematopoietic progenitors, are usually considered as HLA class-I and class-II-negative cells. We show here that differentiation induction (with either sodium butyrate, 12-O-tetradecanoyl-phorbol-13-acetate, or teleocidin) or recombinant alpha- or gamma-interferon (IFN) treatment resulted in the augmentation of HLA class-I antigen expression. This augmentation of HLA class-I antigens was also observed in the Burkitt X K562 hybrid cells PUTKO and DUTKO (the latter coming from two presumably HLA-A, B-negative parents). HLA class-I genes are thus functional in K562 cells. In this system, alpha- and gamma-IFN had no clear differentiating capacity, since they were not able to modulate the expression of various hematopoietic markers, as chemical differentiation inducers did. On the other hand, neither differentiation induction nor interferon treatment could induce HLA class-II antigen expression on K562 cells. These molecules could be very faintly induced in PUTKO and DUTKO hybrids, in contrast with strong HLA class-II expression on the B parental lines. Whether these results are due to "lineage infidelity" in K562 cells or whether K562 cells represent the proliferation of HLA class-I-positive class-II-negative hematopoietic cells, with active suppression of HLA class-II antigen expression, is discussed.

Published

1985

33. Clot structure modification by fondaparinux and consequence on fibrinolysis: a new mechanism of antithrombotic activity.

Author

Varin R, Mirshahi S, Mirshahi P, Kierzek G, Sebaoun D, Mishal Z, Vannier JP, Yvonne Borg J, Simoneau G, Soria C, and Soria J

Subjects

Antithrombin III, Fibrin chemistry, Fibrin drug effects, Fibrinolytic Agents pharmacology, Fondaparinux, Kinetics, Protein Conformation drug effects, Thrombin biosynthesis, Tissue Plasminogen Activator pharmacology, Blood Coagulation, Fibrinolysis drug effects, Polysaccharides pharmacology

Abstract

Fondaparinux is a synthetic pentasaccharide consisting of the minimal sequence of heparin which interacts with antithrombin (AT). It represents a new class of selective factor Xa inhibitors without any antithrombin activity. It has been shown to exhibit potent antithrombotic properties in clinical studies. However, the mechanism of its antithrombotic action has not yet been fully established. In the present study it was shown that fondaparinux, used at pharmacological concentration (500 ng/ml), rendered the clot more susceptible to fibrinolysis induced by t-PA: plasma fibrin clots formed in the presence of fondaparinux and perfused with t-PA were degraded at a faster rate than those formed in the absence of fondaparinux. This fibrinolytic activity of fondaparinux is mainly due to a modification of clot structure characterized by a loose fibrin conformation with less branched fibers and the presence of large pores in comparison to control clots which present a tighter conformation. The difference in fibrin structure was responsible for an increase in clot porosity leading to a better availability of t-PA to the fibrin network. It is related to the decrease in thrombin generation, in an AT-dependent pathway. It was also demonstrated that in the presence of exogenous thrombomodulin, the inhibition of TAFI activation by fondaparinux could contribute, to a lesser extent, to the increased thrombus lysis. The increase in t-PA induced thrombus lysis could contribute to the antithrombotic activity of fondaparinux.

Published

2007

34. Characterization of Brucella abortus lipopolysaccharide macrodomains as mega rafts.

Author

Lapaque N, Forquet F, de Chastellier C, Mishal Z, Jolly G, Moreno E, Moriyon I, Heuser JE, He HT, and Gorvel JP

Subjects

Animals, Cholesterol metabolism, Female, Fluorescence Polarization, Histocompatibility Antigens Class II metabolism, In Vitro Techniques, Lipopolysaccharides pharmacology, Lipopolysaccharides ultrastructure, Macrophages, Peritoneal metabolism, Macrophages, Peritoneal ultrastructure, Membrane Fluidity, Membrane Microdomains ultrastructure, Mice, Mice, Inbred C57BL, Microscopy, Electron, Transmission, beta-Cyclodextrins pharmacology, Brucella abortus metabolism, Lipopolysaccharides metabolism, Membrane Microdomains metabolism

Abstract

The lipopolysaccharides (LPS) of intracellular Proteobacteria such as Brucella, Chlamydia, Legionella and Rickettsia, have properties distinct from enterobacterial LPSs. These properties include deficient LPS induction of host cell activation, low endotoxicity and resistance to macrophage degradation. Together these constitute key virulence mechanisms for intracellular survival and replication. We previously demonstrated that B. abortus LPS captured by macrophages was recycled back to the plasma membrane where it was found associated with macrodomains. Furthermore, this LPS interferes with the MHC class II (MHC-II) presentation of peptides to specific T cell hybridomas. Here, we characterized the Brucella LPS macrodomains by microscopy and biochemistry approaches. We show for the first time that LPS macrodomains act as detergent resistant membranes (DRMs), segregating several lipid-raft components, LPS-binding proteins and MHC-II molecules. Brucella LPS macrodomains remain intact for several months in macrophages and are resistant to the disruptive effects of methyl beta-cyclodextrin. Fluorescent anisotropy measurements show that B. abortus LPS is responsible for the formation of rigid surface membrane complexes. In addition, relocalization of MHC-II molecules is observed in these structures. The effects of B. abortus LPS on membrane properties could be responsible for pathogenic effects such as the inhibition of MHC-II-dependent antigen presentation.

Published

2006

35. Long-term incubation with IL-4 and IL-10 oppositely modifies procoagulant activity of monocytes and modulates the surface expression of tissue factor and tissue factor pathway inhibitor.

Author

Paysant J, Soria C, Cornillet-Lefèbvre P, Nguyen P, Lenormand B, Mishal Z, Vannier JP, and Vasse M

Subjects

Antibodies, Monoclonal immunology, Cells, Cultured, Cytoplasm metabolism, Dose-Response Relationship, Drug, Enzyme-Linked Immunosorbent Assay methods, Gene Expression, Humans, Lipoproteins antagonists & inhibitors, Lipoproteins genetics, Lipoproteins metabolism, Microscopy, Confocal, Monocytes metabolism, RNA, Messenger genetics, Reverse Transcriptase Polymerase Chain Reaction methods, Thromboplastin genetics, Time Factors, Blood Coagulation Factors metabolism, Interleukin-10 pharmacology, Interleukin-4 pharmacology, Monocytes drug effects, Thromboplastin metabolism

Abstract

Monocytes can be induced to express both tissue factor (TF) and its inhibitor, TF pathway inhibitor-1 (TFPI-1). A short incubation (<6 h) with interleukin (IL)-4 and IL-10, two potent deactivators of monocyte functions, has been shown to modulate the synthesis and expression of TF by monocytes activated by lipopolysaccharide, but the consequences of longer incubations (up to 96 h) on both TF and TFPI-1 are unknown. The results of this study showed that adherent monocytes in culture spontaneously expressed TF and TFPI and that prolonged incubation with IL-10 induced a time- and dose-dependent decrease of monocyte TF synthesis, and an accumulation of TF/TFPI-1 complexes at the moncyte surface, suggesting a decreased clearance of these complexes. In contrast, IL-4 induced a time- and dose-dependent increase in TF synthesis, which remained intracytoplasmic, as shown by confocal microscopy. Surprisingly, TF:antigen (Ag) was decreased at the monocyte surface, but the procoagulant activity (PCA) of IL-4-treated monocytes was increased, as a result of more pronounced decrease of TFPI-1:Ag expression than that of TF. In conclusion, prolonged incubation with IL-4 and IL-10 oppositely modified PCA of cultured monocytes, and altered TF and TFPI trafficking and clearance. These data explain the respective deleterious or benefit effects of IL-4 or IL-10 in atherothrombosis.

Published

2005

36. HDAC4 mediates transcriptional repression by the acute promyelocytic leukaemia-associated protein PLZF.

Author

Chauchereau A, Mathieu M, de Saintignon J, Ferreira R, Pritchard LL, Mishal Z, Dejean A, and Harel-Bellan A

Subjects

Animals, HeLa Cells, Humans, Immunohistochemistry, Kruppel-Like Transcription Factors, Mice, NIH 3T3 Cells, Neoplasm Proteins physiology, Oncogene Proteins, Fusion physiology, Promyelocytic Leukemia Zinc Finger Protein, DNA-Binding Proteins physiology, Histone Deacetylases physiology, Leukemia, Promyelocytic, Acute metabolism, Repressor Proteins physiology, Transcription Factors physiology, Transcription, Genetic physiology

Abstract

PLZF, the promyelocytic leukaemia zinc-finger protein, is a transcriptional repressor essential to development. In some acute leukaemias, a chromosomal translocation fusing the PLZF gene to that encoding the retinoic acid receptor RARalpha gives rise to a fusion protein, PLZF-RARalpha, thought to be responsible for constitutive repression of differentiation-associated genes in these cells. Repression by both PLZF and PLZF-RARalpha is sensitive to the histone deacetylase inhibitor TSA, and PLZF was previously shown to interact physically with HDAC1, a class I histone deacetylase. We here asked whether class II histone deacetylases, known to be generally involved in differentiation processes, participate in the repression mediated by PLZF and PLZF-RARalpha, and found that PLZF interacts with HDAC4 in both GST-pull-down and co-immunoprecipitation assays. Furthermore, HDAC4 is indeed involved in PLZF and PLZF-RARalpha-mediated repression, since an enzymatically dead mutant of HDAC4 released the repression, as did an siRNA that blocks HDAC4 expression. Taken together, our data indicate that recruitment of HDAC4 is necessary for PLZF-mediated repression in both normal and leukaemic cells.

Published

2004

37. Dose-dependent effect of dehydroepiandrosterone, but not of its sulphate ester, on angiogenesis.

Author

Varet J, Vincent L, Akwa Y, Mirshahi P, Lahary A, Legrand E, Opolon P, Mishal Z, Baulieu EE, Soria J, Soria C, and Li H

Subjects

Cells, Cultured, Dose-Response Relationship, Drug, Endothelial Cells cytology, Humans, Angiogenesis Inhibitors pharmacology, Dehydroepiandrosterone pharmacology, Dehydroepiandrosterone Sulfate pharmacology, Endothelial Cells drug effects

Abstract

Although dehydroepiandrosterone (DHEA) is widely used in the elderly to prevent some adverse effects of ageing, possible deleterious side effects have not been fully assessed. We evaluated the direct actions of DHEA and DHEA sulphate on angiogenesis, a critical event in pathologies that are common in the elderly (cancer, atherosclerosis, inflammation... etc.). At physiological concentrations found in human plasma following DHEA therapy (1-50 nM), DHEA had no action on angiogenesis in vitro. In contrast, higher concentrations of DHEA (10-100 microM), which can be found in tissues after local administration or storage, inhibited in vitro endothelial cell proliferation (blockage in G2/M), migration and capillary tube formation and in vivo angiogenesis in the Matrigel plug assay. This inhibition might be due to a decreased glucose-6-phosphate dehydrogenase activity and to a modification of the tubulin network involved in cell proliferation and migration. The sulphate ester form of DHEA had no effect on angiogenesis.

Published

2004

38. Scrg1, a novel protein of the CNS is targeted to the large dense-core vesicles in neuronal cells.

Author

Dandoy-Dron F, Griffond B, Mishal Z, Tovey MG, and Dron M

Subjects

Amino Acid Sequence, Animals, Antibodies, Blotting, Western, Cell Line, Central Nervous System chemistry, Chromogranins, DNA, Complementary, Immunohistochemistry, Membrane Glycoproteins analysis, Mice, Microscopy, Immunoelectron, Molecular Sequence Data, Nerve Tissue Proteins genetics, Nerve Tissue Proteins immunology, Proteins analysis, Recombinant Proteins analysis, Synaptotagmins, Calcium-Binding Proteins, Nerve Tissue Proteins analysis, Neurons chemistry, Synaptic Vesicles chemistry

Abstract

Scrapie responsive gene one (Scrg1) is a novel transcript discovered through identification of the genes associated with or responsible for the neurodegenerative changes observed in transmissible spongiform encephalopathies. Scrg1 mRNA is distributed principally in the central nervous system and the cDNA sequence predicts a small cysteine-rich protein 98 amino acids in length, with a N-terminal signal peptide. In this study, we have generated antibodies against the predicted protein and revealed expression of a predominant immunoreactive protein of 10 kDa in mouse brain by Western blot analysis. We have established CAD neuronal cell lines stably expressing Scrg1 to determine its subcellular localization. Several lines of evidence show that the protein is targeted to dense-core vesicles in these cells. (i) Scrg1 is detected by immunocytochemistry as very punctate signals especially in the Golgi apparatus and tips of neurites, suggesting a vesicular localization for the protein. Moreover, Scrg1 exhibits a high degree of colocalization with secretogranin II, a dense-core vesicle marker and a very limited colocalization with markers for small synaptic vesicles. (ii) Scrg1 immunoreactivity is associated with large secretory granules/dense-core vesicles, as indicated by immuno-electron microscopy. (iii) Scrg1 is enriched in fractions of sucrose density gradient where synaptotagmin V, a dense-core vesicle-associated protein, is also enriched. The characteristic punctate immunostaining of Scrg1 is observed in N2A cells transfected with Scrg1 and for the endogenous protein in cultured primary neurons, attesting to the generality of the observations. Our findings strongly suggest that Scrg1 is associated with the secretory pathway of neuronal cells.

Published

2003

39. Identification and characterization of p100HB, a new mutant form of p100/NF-kappa B2.

Author

Derudder E, Laferté A, Ferreira V, Mishal Z, Baud V, Tarantino N, and Körner M

Subjects

Active Transport, Cell Nucleus, Adaptor Proteins, Signal Transducing, Base Sequence, Blotting, Western, Carrier Proteins chemistry, Codon, Dimerization, Exons, Gene Expression Regulation, Humans, I-kappa B Proteins metabolism, Jurkat Cells, Lymphocytes metabolism, Microscopy, Confocal, Molecular Sequence Data, NF-kappa B p52 Subunit, Plasmids metabolism, Point Mutation, Precipitin Tests, Protein Structure, Tertiary, Protein Transport, RNA, Messenger metabolism, Time Factors, Transfection, Tumor Cells, Cultured, Mutation, NF-kappa B chemistry, NF-kappa B genetics

Abstract

P100, which is encoded by NF-kappa B2, inhibits Rel dimers. It can also be processed into p52, one of the DNA binding sub-units of NF-kappa B/Rel factors. Several p100 C-terminal truncations that result from gene rearrangements are associated with lymphomagenesis. Here, we characterized a new p100 mutant that we termed p100HB. It originates from a point-mutation that generates a premature stop-codon, and thus the protein lacks the last 125 amino acids. We have detected p100HB in several human tumor cell lines. The truncated protein is mainly unprocessed, and although it still binds Rel dimers, it has reduced inhibitory potency compared to p100 and translocates into the nucleus. Thus, p100HB may be associated with deregulated NF-kappa B/Rel functions.

Published

2003

40. Endostatin exhibits a direct antitumor effect in addition to its antiangiogenic activity in colon cancer cells.

Author

Dkhissi F, Lu H, Soria C, Opolon P, Griscelli F, Liu H, Khattar P, Mishal Z, Perricaudet M, and Li H

Subjects

Animals, Apoptosis, Cell Cycle, Cell Division, Colonic Neoplasms blood supply, Colonic Neoplasms pathology, Endostatins, Endothelium, Vascular cytology, Female, Flow Cytometry, Genetic Vectors, Humans, Integrin alpha5beta1 genetics, Integrin alpha5beta1 metabolism, Integrin alphaV genetics, Integrin alphaV metabolism, Mice, Mice, Inbred BALB C, Microscopy, Confocal, Neovascularization, Pathologic, Tumor Cells, Cultured, Adenoviridae genetics, Angiogenesis Inhibitors, Antineoplastic Agents, Collagen genetics, Colonic Neoplasms therapy, Peptide Fragments genetics

Abstract

Endostatin has been considered a highly specific inhibitor of endothelial cell proliferation and/or migration. To explore the use of endostatin in antiangiogenic gene therapy, we generated a recombinant adenovirus, AdEndo, carrying the gene for mouse endostatin. Injection of 10(9) PFU of AdEndo resulted in a low but significant suppression (25%) of preestablished tumor growth in murine models involving murine Lewis lung carcinoma (LLC) and human breast cancer MDA-MB-231 tumors. Greater anticancer activity was observed when the same dose of AdEndo was injected into two other preestablished murine models involving C51 murine colon cancer and HT29 human colon cancer (55 and 47% tumor growth reduction, respectively). In vitro, endostatin derived from AdEndo-infected MRC-5 fibroblasts inhibited the growth of C51 and HT29 cell lines (72 and 61%, respectively). The extent of this inhibition was comparable to that observed in endothelial cells: 75% for microcapillary endothelial cell line HMEC-1, 52% for human dermal microvascular endothelial cells, 46% for human umbilical vein endothelial cells, and 67% for calf pulmonary arterial endothelial cells. Both endothelial and colon cancer cells showed a clear increase in cell apoptosis (4- to 5-fold for endothelial cells and 5- to 10-fold for colon cancer cells) and an accumulation in the G(1) phase of the cell cycle. This antiproliferative activity was not observed in other tumor cell lines: LLC, MDA-MB-231, murine colon adenocarcinoma MC38, human prostate cancer cell line DU145, and human breast cancer cell line CAL51. Taken together, these results provide evidence that, in addition to its antiangiogenic activity, endostatin exerts a direct anticancer action that appears to be restricted to some tumor cell lines. Thus, endostatin could be used in some colon cancer treatments and its clinical efficacy would depend on the response of tumor cells themselves.

Published

2003

41. Fenofibrate inhibits angiogenesis in vitro and in vivo.

Author

Varet J, Vincent L, Mirshahi P, Pille JV, Legrand E, Opolon P, Mishal Z, Soria J, Li H, and Soria C

Subjects

Actins metabolism, Apoptosis drug effects, Capillaries drug effects, Capillaries growth & development, Cell Cycle drug effects, Cell Line, Cyclooxygenase 2, Dermis drug effects, Dermis growth & development, Endothelium drug effects, Endothelium growth & development, Humans, In Vitro Techniques, Isoenzymes biosynthesis, Isoenzymes genetics, Membrane Proteins, Prostaglandin-Endoperoxide Synthases biosynthesis, Prostaglandin-Endoperoxide Synthases genetics, Proto-Oncogene Proteins drug effects, Proto-Oncogene Proteins c-akt, Fenofibrate pharmacology, Hypolipidemic Agents pharmacology, Neovascularization, Pathologic drug therapy, Protein Serine-Threonine Kinases

Abstract

Fenofibrate, a peroxisome proliferator-activated receptor (PPAR)-alpha activator, used as a normolipidemic agent, is thought to offer additional beneficial effects in atherosclerosis. Since angiogenesis is involved in plaque progression, hemorrhage, and instability, the main causes of ischemic events, this study was designed to evaluate the action of fenofibrate on angiogenesis. Our results show that fenofibrate (i) inhibits endothelial cell proliferation induced by angiogenic factors, followed at high concentrations by an increase in apoptosis, (ii) inhibits endothelial cell migration in a healing wound model, (iii) inhibits capillary tube formation in vitro, and (iv) inhibits angiogenesis in vivo. Concerning the mechanism of action, the inhibition of endothelial cell migration by fenofibrate can be explained by a disorganization of the actin cytoskeleton. At the molecular level, fenofibrate markedly decreased basic fibroblast growth factor-induced Akt activation and cyclooxygenase 2 gene expression. This inhibition of angiogenesis could participate in the beneficial effect of fenofibrate in atherosclerosis.

Published

2003

42. Processing of filamentous bacteriophage virions in antigen-presenting cells targets both HLA class I and class II peptide loading compartments.

Author

Gaubin M, Fanutti C, Mishal Z, Durrbach A, De Berardinis P, Sartorius R, Del Pozzo G, Guardiola J, Perham RN, and Piatier-Tonneau D

Subjects

Antigen Presentation, B-Lymphocytes metabolism, B-Lymphocytes virology, Bacteriophage M13 immunology, Fluorescein-5-isothiocyanate metabolism, Fluorescent Dyes, Histocompatibility Antigens Class I metabolism, Histocompatibility Antigens Class II metabolism, Humans, Microscopy, Confocal, T-Lymphocytes, Cytotoxic metabolism, T-Lymphocytes, Cytotoxic virology, B-Lymphocytes immunology, Bacteriophage M13 physiology, T-Lymphocytes, Cytotoxic immunology

Abstract

Virions of filamentous bacteriophage fd are capable of displaying multiple copies of peptide epitopes and generating powerful immune responses to them. To investigate the antigen processing mechanisms in human B cell lines used as antigen presenting cells, the major coat protein (pVIII) in intact virions was fluorescently labeled, and its localization in various intracellular compartments was followed using confocal microscopy. We show that the virions were taken up and processed to yield peptides that reach both the major histocompatibility complex (MHC) class II compartment and the endoplasmic reticulum. Moreover, when exposed to bacteriophages displaying a cytotoxic T lymphocyte (CTL) epitope from the reverse transcriptase of human immunodeficiency virus type-1 (HIV-1), B cells were lysed by specific cytotoxic lymphocytes. This confirms that filamentous bacteriophage virions are capable of being taken up and processed efficiently by MHC class I and class II pathways, even in nonprofessional antigen presenting cells. These remarkable features explain, at least in part, the unexpected ability of virions displaying foreign T-cell epitopes to prime strong T-helper-dependent CTL responses. These findings have important implications for the development of peptide-based vaccines, using filamentous bacteriophage virions as scaffolds.

Published

2003

43. Distribution of furamidine analogues in tumor cells: targeting of the nucleus or mitochondria depending on the amidine substitution.

Author

Lansiaux A, Tanious F, Mishal Z, Dassonneville L, Kumar A, Stephens CE, Hu Q, Wilson WD, Boykin DW, and Bailly C

Subjects

Adenocarcinoma metabolism, Animals, Antineoplastic Agents pharmacology, Base Sequence, Benzamidines chemistry, Benzamidines pharmacology, Cell Division drug effects, DNA, Neoplasm metabolism, HT29 Cells, Humans, Male, Melanoma, Experimental drug therapy, Melanoma, Experimental metabolism, Melanoma, Experimental pathology, Mice, Microscopy, Confocal, Microscopy, Fluorescence, Molecular Sequence Data, Prostatic Neoplasms metabolism, Structure-Activity Relationship, Tumor Cells, Cultured, Antineoplastic Agents pharmacokinetics, Benzamidines pharmacokinetics, Cell Nucleus metabolism, Mitochondria metabolism, Neoplasms metabolism

Abstract

Diphenylfuran diamidines represent an important class of DNA minor groove binders of high therapeutic interest as antiparasitic or antitumor agents depending on the compounds structures. To exert their cytotoxic action, the compounds must first get into the cell and reach the nuclear compartment where the main target, DNA, is located. The forces that drive the drugs into cell nuclei, as well as the influence of the molecular structures on the cell distribution, are not known. To address these issues, we took advantage of the fluorescence of the molecules to analyze their intracellular distribution profiles in tumor cells of different origins (B16 melanoma, MCF7 mammary adenocarcinoma, A549 lung carcinoma, HT29 colon carcinoma, LNCaP, and PC3 prostatic carcinoma) by epifluorescence and confocal microscopy. A homogeneous series of synthetic bis-substituted alkyl or phenyl amidine and reverse amidine derivatives of furamidine was used to dissect the molecular mechanisms that control the distribution of the drugs into the cytoplasm or the nucleus of the cells. The amidine (DB75) and the various N-alkyl derivatives were found to accumulate selectively in the cell nuclei. This is also the case for a guanidine derivative but not for the phenyl-substituted compound DB569, which essentially localizes in cytoplasmic granules. Similar cytoplasmic patterns were observed with a reverse amidine analogue and a pyridine-substituted compound indicating that the presence of aromatic rings on the terminal side chain is the limiting factor that restricts the uptake of the compounds in the nuclear compartment. The use of different organelle-selective fluorescent probes, such as JC-1 and chloromethyl-X-rosamine, both specific to mitochondria and neutral red considered as a lysosome-selective probe, suggests that DB569 preferentially accumulates in mitochondria. Competition experiments with the antitumor drug daunomycin reveal that the diphenylfurans are attracted into the nuclei by the DNA. The DNA minor groove-drug interactions provide the driving force that permits massive accumulation of the fluorescent molecules in the nuclei. The DNA binding properties of the diphenylfuran derivatives were investigated by DNase I footprinting and surface plasmon resonance biosensor experiments to measure sequence selectivity and binding affinities, respectively. Furamidine and its phenyl-substituted analogue that accumulate in the cell nuclei and mitochondria, respectively, share a common selectivity for AT sites and bind equally tightly to these sites. Therefore, it is possible to modulate the intracellular distribution of the furamidine derivatives without affecting their DNA binding and sequence recognition properties. The introduction of aromatic substituents on diphenylfuran diamidines represents a novel strategy to control the intracellular compartmentalization of these DNA binding agents and directs them to mitochondria. This drug design strategy may prove useful to trigger drug-induced apoptosis.

Published

2002

44. Engagement of the inhibitory receptor CD158a interrupts TCR signaling, preventing dynamic membrane reorganization in CTL/tumor cell interaction.

Author

Guerra N, Michel F, Gati A, Gaudin C, Mishal Z, Escudier B, Acuto O, Chouaib S, and Caignard A

Subjects

Calcium metabolism, Humans, Killer Cells, Natural immunology, Membrane Microdomains immunology, Microscopy, Confocal, Phosphorylation, Receptors, Antigen, T-Cell antagonists & inhibitors, Receptors, KIR, Receptors, KIR2DL1, Tumor Cells, Cultured, Carcinoma, Renal Cell immunology, Cell Membrane immunology, Kidney Neoplasms immunology, Receptors, Antigen, T-Cell immunology, Receptors, Immunologic immunology, T-Lymphocytes, Cytotoxic immunology

Abstract

Renal cell carcinoma (RCC) infiltrating lymphocytes (TILs) express killer cell immunoglobulinlike receptors (KIRs) that inhibit the antitumor CD8(+) T-cell lysis. In the present study, to better examine the functional consequences of KIR engagement on cytotoxic T lymphocyte (CTL)/tumor interaction, we have investigated the influence of KIR CD158a on early steps of T-cell activation. We show that coengagement of T-cell receptor (TCR) and CD158a by tumor cells inhibited tyrosine phosphorylation of early signaling proteins ZAP-70 and LAT, lipid raft coalescence, and TCR/CD3 accumulation at the CTL/tumor cell interface. In addition, the guanine exchange factor Vav was not phosphorylated, and no actin cytoskeleton rearrangement was observed. Our data indicate a role of KIR CD158a in the dynamic events induced by TCR triggering, preventing CTL membrane reorganization, and subsequent completion of CTL activation program. Accordingly, the expression of CD158 by TILs may favor tumor cell escape to the immune response.

Published

2002

45. Treatment of cancer cells with methioninase produces DNA hypomethylation and increases DNA synthesis.

Author

Machover D, Zittoun J, Saffroy R, Broët P, Giraudier S, Magnaldo T, Goldschmidt E, Debuire B, Orrico M, Tan Y, Mishal Z, Chevallier O, Tonetti C, Jouault H, Ulusakarya A, Tanguy ML, Metzger G, and Hoffman RM

Subjects

DNA, Neoplasm genetics, DNA, Neoplasm metabolism, Dose-Response Relationship, Drug, Humans, Kinetics, Leukemia, T-Cell genetics, Leukemia, T-Cell metabolism, Recombinant Proteins pharmacology, Tumor Cells, Cultured, Antimetabolites, Antineoplastic pharmacology, Carbon-Sulfur Lyases pharmacology, DNA Methylation drug effects, DNA, Neoplasm biosynthesis, Leukemia, T-Cell drug therapy

Abstract

Methionine depletion in the human cell line CCRF-CEM through the action of recombinant methioninase (rMETase), a methionine-cleaving enzyme, was previously demonstrated to produce a strong cytotoxic synergistic effect with fluorouracil (FUra) throughout a broad range of concentrations of FUra and rMETase, including subcytotoxic levels of rMETase. Potentiation was associated with a decrease in free thymidylate synthase from preexisting levels. To further investigate the action of rMETase on CCRF-CEM cells, in the present study we explored the effects of rMETase as a single agent on DNA methylation levels and DNA synthesis, which may be changed as a result of deprivation of methionine. Cells treated with rMETase under subcytotoxic conditions contained significantly lower levels of genomic methylated DNA than did control cells, as demonstrated by incorporation of the methyl radical of [methyl-(3)H]S-adenosylmethionine in DNA and by use of methylation-sensitive arbitrarily primed PCR. DNA hypomethylation produced by rMETase was of similar magnitude as that produced with the DNA methyltransferase inhibitor 5-azacytidine. Cells exposed to rMETase synthesized significantly more DNA than did untreated cells. Incorporation of [6-3H]thymidine and [6-3H]2'-deoxyuridine in these cells was augmented over that in control by mean factors of 1.78 and 2.36, respectively. Increased 3H nucleoside incorporation resulted in greater numbers of nuclear grains as demonstrated by autoradiography. The increase in DNA synthesis induced by rMETase is likely to result from enhancement of DNA repair because it was not accompanied by differences in cell cycle phase distribution or in total DNA content as determined by flow cytometry. We hypothesize that potentiation of FUra cytotoxicity by rMETase may result from increased inhibition of thymidylate synthase, together with DNA hypomethylation and enhanced DNA repair that could be involved in cell responses to drug-induced damage.

Published

2002

46. Cerivastatin, an inhibitor of 3-hydroxy-3-methylglutaryl coenzyme a reductase, inhibits endothelial cell proliferation induced by angiogenic factors in vitro and angiogenesis in in vivo models.

Author

Vincent L, Soria C, Mirshahi F, Opolon P, Mishal Z, Vannier JP, Soria J, and Hong L

Subjects

Arteriosclerosis pathology, Arteriosclerosis prevention & control, Cell Division drug effects, Cyclin-Dependent Kinase Inhibitor p21, Cyclins metabolism, Endothelium, Vascular cytology, G1 Phase drug effects, Humans, Microcirculation, Neovascularization, Pathologic prevention & control, Polyisoprenyl Phosphates metabolism, Polyisoprenyl Phosphates pharmacology, Sesquiterpenes, Signal Transduction drug effects, rhoA GTP-Binding Protein metabolism, Endothelium, Vascular drug effects, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Pyridines pharmacology

Abstract

Cerivastatin is an inhibitor of 3-hydroxy-3-methylglutaryl coenzyme A reductase. It inhibits the biosynthesis of cholesterol and its precursors: farnesyl pyrophosphate and geranylgeranyl pyrophosphate (GGPP), which are involved in Ras and RhoA cell signaling, respectively. Statins induce greater protection against vascular risk than that expected by cholesterol reduction. Therefore, cerivastatin could protect plaque against rupture, an important cause of ischemic events. In this study, the effect of cerivastatin was tested on angiogenesis because it participates in plaque progression and plaque destabilization. Cerivastatin inhibits in vitro the microvascular endothelial cell proliferation induced by growth factors, whereas it has no effect on unstimulated cells. This growth arrest occurs at the G(1)/S phase and is related to the increase of the cyclin-dependent kinase inhibitor p21(Waf1/Cip1). These effects are reversed by GGPP, suggesting that the inhibitory effect of cerivastatin is related to RhoA inactivation. This mechanism was confirmed by RhoA delocalization from cell membrane to cytoplasm and actin fiber depolymerization, which are also prevented by GGPP. It was also shown that RhoA-dependent inhibition of cell proliferation is mediated by the inhibition of focal adhesion kinase and Akt activations. Moreover, cerivastatin inhibits in vivo angiogenesis in matrigel and chick chorioallantoic membrane models. These results demonstrate the antiangiogenic activity of statins and suggest that it may contribute to their therapeutic benefits in the progression and acute manifestations of atherosclerosis.

Published

2002

47. Cerivastatin, an inhibitor of HMG-CoA reductase, inhibits the signaling pathways involved in the invasiveness and metastatic properties of highly invasive breast cancer cell lines: an in vitro study.

Author

Denoyelle C, Vasse M, Körner M, Mishal Z, Ganné F, Vannier JP, Soria J, and Soria C

Subjects

Apoptosis drug effects, Base Sequence, Cell Cycle drug effects, Cell Division drug effects, Cyclin-Dependent Kinase Inhibitor p21, Cyclins genetics, DNA Primers, Humans, I-kappa B Proteins metabolism, In Vitro Techniques, Matrix Metalloproteinase 9 metabolism, NF-kappa B antagonists & inhibitors, RNA, Messenger genetics, Thromboplastin metabolism, Tumor Cells, Cultured, Urokinase-Type Plasminogen Activator metabolism, Breast Neoplasms pathology, Gene Expression Regulation, Neoplastic drug effects, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Neoplasm Invasiveness, Neoplasm Metastasis, Pyridines pharmacology, Signal Transduction drug effects

Abstract

Cerivastatin is used in the treatment of hypercholesterolemia to inhibit 3-hydroxy 3-methylglutaryl coenzyme A reductase and thus prevent the synthesis of cholesterol precursors, such as farnesyl pyrophosphate (FPP) and geranylgeranyl pyrophosphate (GGPP), responsible, respectively, for translocation of Ras and Rho to the cell membrane, a step required for their cell signaling, leading to cell proliferation and migration. Recently, it has been suggested that non lipid-related effects of statins could play a beneficial role in cancer therapy. In this study, we have investigated the mechanisms by which statins inhibit cancer and the types of cancers which could benefit from this therapy. In MDA-MB-231 cells, an aggressive breast cancer cell line with spontaneous activation of Ras and NFkappaB and overexpression of RhoA, cerivastatin induced inhibition of both cell proliferation and invasion through Matrigel. This anti-proliferative effect was related to G(1)/S arrest due to an increase in p21(Waf1/Cip1). The anti-invasive effect was observed from 18 h and could be explained by RhoA delocalization from the cell membrane, resulting in disorganization of the actin fibers and disappearance of focal adhesion sites. The importance of RhoA inactivation in both these inhibitory effects was proved by their reversion by GGPP but not by FPP. Moreover, cerivastatin was also shown to induce inactivation of NFkappaB, in a RhoA inhibition-dependent manner, resulting in a decrease in urokinase and metalloproteinase-9 expression, two proteases involved in cell migration. The participation of Ras inactivation is considered a subsidiary mechanism for the effects of cerivastatin, as they were not rescued by FPP. Prolonged treatment of MDA-MB-231 cells with high doses of cerivastatin induced a loss of cell attachment. Interestingly, the effect of cerivastatin was considerably lower on poorly invasive MCF-7 cells. In conclusion, our results suggest that cerivastatin inhibits cell signaling pathways involved in the invasiveness and metastatic properties of highly invasive cancers.

Published

2001

48. Effects of Abciximab on the architecture of platelet-rich clots in patients with acute myocardial infarction undergoing primary coronary intervention.

Author

Collet JP, Montalescot G, Lesty C, Mishal Z, Soria J, Choussat R, Drobinski G, Soria C, Pinton P, Barragan P, and Thomas D

Subjects

Abciximab, Aged, Blood Platelets chemistry, Blood Platelets drug effects, Double-Blind Method, Female, Humans, Male, Myocardial Infarction blood, Platelet Aggregation drug effects, Treatment Outcome, Viscosity drug effects, Antibodies, Monoclonal therapeutic use, Blood Coagulation drug effects, Blood Platelets metabolism, Immunoglobulin Fab Fragments therapeutic use, Myocardial Infarction therapy, Platelet Aggregation Inhibitors therapeutic use

Abstract

Background: Abciximab plus aspirin improves the TIMI 3 flow rate of the infarct-related artery in patients treated with either percutaneous coronary intervention or thrombolysis. The present study investigated whether the reperfusion efficacy of abciximab relates to modifications of clot architecture in patients admitted for acute myocardial infarction (AMI)., Methods and Results: A total of 23 AMI patients in the Abciximab before Direct angioplasty and stenting in Myocardial Infarction Regarding Acute and Long term follow-up (ADMIRAL) trial received, in a double-blind fashion, either abciximab (n=13) or placebo (n=10) before primary stenting. Viscoelastic (G' in dyne/cm(2)) and morphological (mean platelet aggregate surface area [SAG] in micrometer(2)) indexes of ex vivo platelet-rich clots (PRC) were assessed in a double-blind fashion before and after the bolus administration of abciximab or placebo. G' and SAG reflect the mechanical and morphological impact of activated platelets on the PRC fibrin network, respectively. Abciximab administration reduced G' by 63% (P=0.0001) and SAG by 65% (P=0.0007), and no effect was seen in the placebo group. These abciximab-related changes increased fibrin exposure as a consequence of the platelet-aggregate surface reduction and may have improved endogenous fibrinolysis. These effects were identified in all patients, independent of previous heparin administration., Conclusions: Abciximab dramatically reduces platelet aggregate size and increases the fibrin accessibility of ex vivo PRC in AMI patients. These modifications could participate in the better coronary artery patency observed with abciximab.

Published

2001

49. Inhibition of endothelial cell migration by cerivastatin, an HMG-CoA reductase inhibitor: contribution to its anti-angiogenic effect.

Author

Vincent L, Chen W, Hong L, Mirshahi F, Mishal Z, Mirshahi-Khorassani T, Vannier JP, Soria J, and Soria C

Subjects

Actins metabolism, Cell Line, Cell Membrane metabolism, Endothelial Growth Factors pharmacology, Endothelium, Vascular physiology, Fibroblast Growth Factor 2 pharmacology, Humans, Lymphokines pharmacology, Matrix Metalloproteinase 2 biosynthesis, Matrix Metalloproteinase 2 genetics, Oncostatin M, Peptides pharmacology, Polyisoprenyl Phosphates pharmacology, Polymers metabolism, RNA, Messenger biosynthesis, Sesquiterpenes, Vascular Endothelial Growth Factor A, Vascular Endothelial Growth Factors, Wound Healing, rhoA GTP-Binding Protein metabolism, Cell Movement drug effects, Endothelium, Vascular drug effects, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Neovascularization, Physiologic drug effects, Pyridines pharmacology

Abstract

Recent studies have suggested that inhibitors of 3-hydroxy-3-methyl-glutaryl-coenzyme A reductase (statins) can play a role in protection against vascular risk, which is independent of cholesterol reduction. It could act by inhibiting the synthesis of isoprenoids (farnesylpyrophosphate (FPP) and geranylgeranylpyrophosphate (GGPP)), which are respectively essential for membrane attachment and biological activity of GTPases Ras and RhoA. This study demonstrates that a statin (cerivastatin) inhibits angiogenesis. This effect was due to a decrease in endothelial cell locomotion which was reversed by GGPP. It was mainly related to delocalization of RhoA from cell membrane to cytoplasm, responsible for the disorganization of actin stress fibers. Furthermore, a decrease in MMP-2 secretion, involved in cell invasion, was also observed. This effect is rather due to Ras inhibition as it was reversed by FPP. This anti-angiogenic activity could explain the beneficial effect of statins on atherosclerosis and on cancer prevention as shown by clinical studies.

Published

2001

50. CD9 and megakaryocyte differentiation.

Author

Clay D, Rubinstein E, Mishal Z, Anjo A, Prenant M, Jasmin C, Boucheix C, and Le Bousse-Kerdilès MC

Subjects

ADP-ribosyl Cyclase, ADP-ribosyl Cyclase 1, Antibodies, Monoclonal immunology, Antibodies, Monoclonal pharmacology, Antigens, CD biosynthesis, Antigens, CD genetics, Antigens, CD immunology, Antigens, Differentiation biosynthesis, B-Lymphocytes cytology, Cell Differentiation, Cell Lineage, Cell Membrane immunology, Cell Membrane ultrastructure, Cells, Cultured, Colony-Forming Units Assay, Flow Cytometry, Gene Expression Regulation, Developmental, Humans, Immunophenotyping, Megakaryocytes metabolism, Megakaryocytes ultrastructure, Microscopy, Electron, NAD+ Nucleosidase biosynthesis, Platelet Glycoprotein GPIIb-IIIa Complex biosynthesis, Tetraspanin 29, Antigens, CD physiology, Megakaryocytes cytology, Membrane Glycoproteins

Abstract

It is shown that the tetraspanin CD9 has a complex pattern of distribution in hematopoietic cells and is heterogeneously expressed on human bone marrow CD34(+) cells. CD34(high)CD38(low)Thy1(+) primitive progenitors are contained in the population with intermediate CD9 expression, thus suggesting that CD9 expression may precede CD38 appearance. Cell sorting shows that colony-forming unit (CFU)-GEMM and CFU-GM are present in high proportions in this fraction and in the fraction with the lowest CD9 expression. Cells with the highest level of CD9 are committed to the B-lymphoid or megakaryocytic (MK) lineages, as shown by the co-expression of either CD19 or CD41/GPIIb and by their strong potential to give rise to CFU-MK. In liquid cultures, CD9(high)CD41(neg) cells give rise to cells with high CD41 expression as early as 2 days, and this was delayed by at least 3 to 4 days for the CD9(mid) cells; few CD41(high) cells could be detected in the CD9(low) cell culture, even after 6 days. Antibody ligation of cell surface CD9 increased the number of human CFU-MK progenitors and reduced the production of CD41(+) megakaryocytic cells in liquid culture. This was associated with a decreased expression of MK differentiation antigens and with an alteration of the membrane structure of MK cells. Altogether these data show a precise regulation of CD9 during hematopoiesis and suggest a role for this molecule in megakaryocytic differentiation, possibly by participation in membrane remodeling. (Blood. 2001;97:1982-1989)

Published

2001