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291 results on '"Andrieu, J. M."'

1. Evidence of a tolerogenic vaccine against AIDS in the Chinese macaque prefigures a potential human vaccine

Author

Andrieu, J. M. and Lu, Wei

Subjects
viruses, animal diseases, virus diseases
Abstract

In 2006 we discovered a new type of mucosal vaccine against simian immunodeficiency virus (SIV) in Chinese macaques. Here, we review 15 years of our published work on this vaccine, which consists of inactivated SIVmac239 particles adjuvanted with Bacillus Calmette-Guerin, Lactobacillus plantarum, or Lactobacillus rhamnosus. Without adjuvant, the vaccine administered by the intragastric route induced the usual SIV-specific humoral and cellular immune responses but provided no protection against intrarectal challenge with SIVmac239. In contrast, out of 24 macaques immunized with the adjuvanted vaccine and challenged intrarectally with SIVmac239 or SIVB670, 23 were sterilely protected for up to five years, while all control macaques were infected. This protection was confirmed by an independent group from the Pasteur Institute. During the past 15 years, we have identified the mechanism of action of the vaccine and discovered that the vaccinated macaques produced a previously unrecognized class of MHC-Ib/E-restricted CD8(+) T cells (which we refer to as tolerogenic CD8(+) T cells) that suppressed the activation of SIV-RNA-infected CD4(+) T cells and thereby inhibited the (activation-dependent) reverse transcription of the virus, which in turn prevented the establishment of SIV infection. Importantly, we discovered also that the tolerogenic CD8(+) T cell subset observed in vaccinated Chinese macaques could also be found in human elite controllers, a small group of HIV-infected patients in whom these tolerogenic CD8(+) T cells were shown to naturally suppress viral replication. Given that SIV and HIV require activated immune cells in which to replicate, the specific prevention of activation of SIV-RNA-containing CD4(+) T cells by a tolerogenic vaccine approach offers an exciting new avenue in HIV vaccine research.

Published
2021

8. Distinctive effects of CCR5, CCR2, and SDF1 genetic polymorphisms in AIDS progression

Author

Hendel, H., Henon, N., Lebuanec, H., Lachgar, A., Poncelet, H., Caillat-Zucman, s., Winkler, C.A., Smith, M.W., Kenefic, L., O'Brien, S., Lu, W., Andrieu, J.-M., Zagury, D., Schachter, F., Rappaport, J., and Zagury, J.-F.

Subjects
Genetic polymorphisms -- Health aspects, HIV infection -- Development and progression, Cell receptors -- Genetic aspects, Health
Abstract

Gene mutations in the cell receptors CCR5 and CCR2 appear to be linked to slow progression of HIV infection. Researchers analyzed gene mutations in the CCR5 and CCR2 cell receptors in 290 HIV-infected people, of whom 200 were non-progressors or slow progressors and 90 were fast progressors. Slow or non-progressors were more likely to have the ccr5-delta32 gene mutation than fast progressors. Slow or non-progressors who did not have a CCR5 mutation were more likely to have a CCR2 mutation.

Published
1998

9. Hepatic safety of ketoconazole in Cushing’s syndrome: results of a Compassionate Use Programme in France

Author

Young, Jacques, primary, Bertherat, Jérôme, additional, Vantyghem, Marie Christine, additional, Chabre, Olivier, additional, Senoussi, Salima, additional, Chadarevian, Rita, additional, Castinetti, Frédéric, additional, _, _, additional, Abeillon, J, additional, Ajzenberg, C, additional, Andrieu, J-M, additional, Arbey, A-S, additional, Archambeaud, F, additional, Arnault, G, additional, Bacchetta, J, additional, Baechler-Sadoul, E, additional, Bakiri, F, additional, Batisse-Lignier, M, additional, Baudry, C, additional, Benamo, E, additional, Bennet, A, additional, Berdelou, A, additional, Bertherat, J, additional, Boehna, A, additional, Borson-Chazot, F, additional, Bourcigaux, N, additional, Bourquard, C, additional, Bouys, L, additional, Bremont-Weill, C, additional, Bricaire, L, additional, Brue, T, additional, Buliga, D, additional, Cabaret, P, additional, Caron, P, additional, Cerro-Martinez, M, additional, Chambre, C, additional, Chardonnet, M, additional, Chatelin, J, additional, Clavel, C, additional, Coffin, C, additional, Cohen, R, additional, Collet-Gaudillat, C, additional, Cortet, C, additional, Coulon, A-L, additional, De Boisvilliers, F, additional, Decker-Bellaton, A, additional, Delemer, B, additional, De Menthon, M, additional, Degros, V, additional, Deneuville, T, additional, Desailloud, R, additional, Di Pietro, G, additional, Do Cao, C, additional, Donadille, B, additional, Dolz, M, additional, Dubray-Longeras, P, additional, Dutertre, E, additional, Du Rostu, H, additional, El Farkh, J, additional, Faure, G, additional, Finichel, P, additional, Gaits, N, additional, Galland, F, additional, Genc, S, additional, Ghanassia, E, additional, Girard, J-J, additional, Gravis, G, additional, Groza, L, additional, Grunenberger, F, additional, Guiheneuf, C, additional, Guignat, L, additional, Guigui, M, additional, Guilhem, A, additional, Joubert, M, additional, Jublanc, C, additional, Kamenicky, P, additional, Kerlan, V, additional, Khalfallah, Y, additional, Lambrey, G, additional, Landau, E, additional, Lautridou, C, additional, Lefebvre, H, additional, Le Bras, M, additional, Le Guillou, A-C, additional, Le Pommelet, C, additional, Léonard, F, additional, Lin, L, additional, Luca, F, additional, Lunogo, C, additional, Maisin, A, additional, Maiza, J-C, additional, Marty, M, additional, Meliani, P, additional, Menon, S, additional, Mestre, B, additional, Mignot, B, additional, Millot, S, additional, Morange, I, additional, Moret, M, additional, Morlet-Barla, N, additional, Narbonne, H, additional, Néraud, B, additional, Néri, N, additional, Niccoli, P, additional, Nunes, M L, additional, Oudard, S, additional, Papadopoulou, S, additional, Petit, J-M, additional, Petit-Aubert, G, additional, Perrin, A, additional, Philippon, M, additional, Pillegrand, C, additional, Potton, L, additional, Raverot, G, additional, Rodes, M L, additional, Reznik, Y, additional, Sadoul, J L, additional, Salenave, S, additional, Saraval-Gross, M, additional, Sarfati, J, additional, Savel, J, additional, Schletzer, M A, additional, Schneebeli, S, additional, Schillo, F, additional, Smagala, A, additional, Sonnet, E, additional, Teissier, R, additional, Tessier, M P, additional, Trulli, F, additional, Vackrine, C, additional, Vezzosi, D, additional, Viard, A, additional, Villeneuve, A, additional, Weryha, G, additional, and Zalzali, M, additional

Published
2018
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11. HIV-Related Hematological Neoplasias in France

Author

Andrieu, J.-M., Toledano, M., Raphael, M., Tourani, J.-M., Desablens, B., Herfarth, Ch., editor, Senn, H.-J., editor, Baum, M., editor, Diehl, V., editor, von Essen, C., editor, Grundmann, E., editor, Hitzig, W., editor, Rajewsky, M. F., editor, Schmid, Luzius, editor, and Senn, Hans-Jörg, editor

Published
1988
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12. Hämatologie

Author

Röcker, L., Franz, I. W., Lohmann, F. W., Gregor, B., Pfreundschuh, M., Dörken, B., Ho, A. D., Körbling, M., Hunstein, W., König, E., Meusers, P., Lang, E., Brittinger, G., Friedrich, G., Leder, L. D., Graubner, M., Löffler, H., Pralle, H., Hans, C., Maas, D., Schöpf, E., Burke, P. J., Elfenbein, G. J., Braine, H. G., Santos, G. W., Wernet, P., Wilms, K., Ziegler, A., Link, H., Meyer, P., Köttgen, E., Fabricius, H. Ä, Stahn, R., Gerok, W., Müller, C., Heinrichs, H., Steinke, B., Waller, H. D., Gamm, H., Preiß, J., Fischer, J., Schniepp, I., Zeile, G., Leser, H. G., Bärlin, E., Weltzien, H. U., Gemsa, D., Ludwig, H., Adolf, G. R., Swetly, P., Schubotz, R., Wacker, H. J., Kaffarnik, H., Heidemann, E., Nerke, O., Weber, S., Raif, W., Bross, K., Heilmann, E., Holzknecht, A., Fahrenkrug, H., Schalhorn, A., Wagner, H., Wilmanns, W., Poutot, G. Stupp, Delbrück, H., Teillet, F., Weissgerber, C. Bayle, Andrieu, J. M., Clot, P. H., Bernard, J., and Miehlke, K., editor

Published
1981
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14. Evolving molecular epidemiological profile of human immunodeficiency virus 1 in the southwest border of China

Author

Chen, Y. Y., Chen, S., Kang, J., Fang, H., Dao, H., Guo, W. Z., Lai, C. H., Lai, M. Y., Fan, J. H., Fu, L. C., Andrieu, J. M., and Lu, Wei

Subjects
virus diseases
Abstract

Background: We have previously reported in Xishuangbanna (Banna) Dai Autonomous Prefecture, a well-developed tourist destination in the southwest border of China, that HIV-1 transmitted dominantly through heterosexual contact with less divergent genotypes and few drug resistant mutations [1]. Due to the rapid increase of newly diagnosed HIV-1 cases per year in Banna in recent years, it's important to evaluate the evolution of HIV-1 molecular epidemiology for the better understanding of ongoing HIV-1 outbreak in this region. Methodology/Principal Findings: By sequencing of HIV-1 pol genes and phylogenetic analysis, we conducted a molecular epidemiologic study in 352 HIV-1-seropositive highly active antiretroviral treatment (HAART)-naive individuals newly diagnosed at the Banna Center for Disease Control and Prevention between 2009 and 2011. Of 283 samples (84.1% taken from heterosexually acquired adults, 10.6% from needle-sharing drug users, 2.8% from men who have sex with men, 0.4% from children born from HIV-1-infected mothers, and 2.1% remained unknown) with successful sequencing for pol gene, we identified 108 (38.2%) HIV-1 subtype CRF08_BC, 101 (35.7%) CRF01_AE, 49 (17.3%) CRF07_BC, 5 (1.8%) C/CRF57_BC, 3 (1.1%) B', 1 (0.4%) B/CRF51_01B, and 16 (5.7%) unique recombinants forms. Among these infected individuals, 104 (36.7%) cases showed drug resistant or resistance-relevant mutations, and 4 of them conferring high-level resistance to 3TC/FTC, EFV/NVP or NFV. Phylogenetic analysis revealed 21 clusters (2-7 sequences) with only 21.2% (60/283) sequences involved. Conclusion/Significance: In contrast to our previous findings, CRF08_BC, replaced CRF01_AE, became the dominant genotype of HIV-1 in Banna prefecture. The viral strains with drug resistance mutations were detected frequently in newly diagnosed HIV-1-infected individuals in this region.

Published
2014

17. Induction of CD8(+) regulatory T cells protects macaques against SIV challenge

Author

Lu, Wei, Chen, S., Lai, C. H., Guo, W. Z., Fu, L. C., and Andrieu, J. M.

Subjects
animal diseases, viruses, virus diseases
Abstract

Efforts to develop a vaccine against HIV have so far met with limited success. Given that CD4(+) T cell activation drives the initial burst of viral replication, we explored in macaques whether an oral vaccine comprised of Lactobacillus plantarum, a commensal bacterium that favors immune tolerance, and inactivated simian immunodeficiency virus mac239 (SIVmac239) would induce CD4(+) T cell unresponsiveness/tolerance toward SIV antigens and thereby prevent the establishment of SIV infection. The tolerogenic vaccine induced MHC-Ib/E-restricted CD8(+) regulatory T cells (Tregs) that suppressed SIV-harboring CD4(+) T cell activation and ex vivo SIV replication in 15 of 16 animals without inducing SIV-specific antibodies or cytotoxic T lymphocytes. Of 16 macaques that were intrarectally challenged with SIVmac239 or heterologous strain SIVB670, 15 were sterilely protected. In four macaques that were rechallenged intravenously, plasma SIV levels peaked slightly and then dropped to undetectable levels, although the animals subsequently harbored intracellular SIV DNA. Infusion of CD8 antibodies confirmed the role of CD8(+) Tregs in preventing/suppressing SIV in vivo. These findings suggest a new avenue of research toward developing an HIV-1 vaccine.

Published
2012

18. Molecular epidemiology of Human Immunodeficiency Virus Type 1 in Guangdong Province of Southern China

Author

Chen, S., Cai, W. P., He, J. Y., Vidal, Nicole, Lai, C. H., Guo, W. Z., He, H. L., Chen, X. J., Fu, L. S., Peeters, Martine, Delaporte, Eric, Andrieu, J. M., and Lu, Louis

Subjects
virus diseases
Abstract

Background: Although the outbreak of human immunodeficiency virus type 1 (HIV-1) in Guangdong has been documented for more than a decade, the molecular characteristics of such a regional HIV-1 epidemic remained unknown. Methodology/Principal Findings: By sequencing of HIV-1 pol/env genes and phylogenetic analysis, we performed a molecular epidemiologic study in a representative subset (n = 200) of the 508 HIV-1-seropositive individuals followed up at the center for HIV/AIDS care and treatment of Guangzhou Hospital of Infectious Diseases. Of 157 samples (54.1% heterosexual acquired adults, 20.4% needle-sharing drug users, 5.7% receivers of blood transfusion, 1.3% men who have sex with men, and 18.5% remained unknown) with successful sequencing for both pol and env genes, 105 (66.9%) HIV-1 subtype CRF01_AE and 24 (15.3%) CRF07_BC, 9 (5.7%) B', 5 (3.2%) CRF08_BC, 5 (3.2%) B, 1 (0.6%) C, 3 (1.9%) CRF02_AG, and 5 (3.2%) inter-region recombinants were identified within pol/env sequences. Thirteen (8.3%) samples (3 naives, 6 and 5 received with antiretroviral treatment [ART] 1-21 weeks and >= 24 weeks respectively) showed mutations conferring resistance to nucleoside/nonnucleoside reverse transcriptase inhibitors or protease inhibitors. Among 63 ART-naive patients, 3 (4.8%) showed single or multiple drug resistant mutations. Phylogenetic analysis showed 8 small clusters (2-3 sequences/cluster) with only 17 (10.8%) sequences involved. Conclusion/Significance: This study confirms that sexual transmission with dominant CRF01_AE strain is a major risk for current HIV-1 outbreak in the Guangdong's general population. The transmission with drug-resistant variants is starting to emerge in this region.

Published
2012

19. Tumor necrosis factor production in HIV-seropositive subjects. Relationship with lung opportunistic infections and HIV expression in alveolar macrophages

Author

Dominique ISRAEL-BIET, Cadranel, J., Beldjord, K., Andrieu, J. -M, Jeffrey, A., and Even, P.

Subjects
Immunology, Immunology and Allergy
Abstract

We have evaluated the TNF production by alveolar macrophages (AM) in 43 HIV-infected subjects in relation with 1) their clinical and biologic status; 2) the presence of lung opportunistic infections (OI); and 3) the expression of HIV by AM. This production was assessed in a standard chromium release test, using monocytic U937 cells as targets. The spontaneous TNF production by AM from patients without lung OI was higher than that from seronegative controls (p less than 0.02). This production by AM was similar to that of blood monocytes, suggesting that it was not related, in these subjects, to any particular lung status. The extent of TNF release by AM was correlated to the presence of a lymphocytic alveolitis (p less than 0.05), and not to the patients' clinical presentation nor to their CD4 cell count. Finally, AM from these subjects could be normally stimulated in vitro by IFN-gamma. On the other hand, it appeared that the spontaneous TNF release by AM shown in vitro to express HIV (p24+ AM) was significantly higher than that by their p24- counterparts (p less than 0.05) and by controls (p less than 0.01). In addition, contrasting with the marked increase of TNF release by p24- AM after their stimulation with IFN-gamma (p less than 0.001), p24+ AM appeared to be refractory to any stimulation by IFN, arguing for their activation in vivo. Finally, the spontaneous TNF release by AM was significantly increased during lung OI, compared with controls (p less than 0.01) as well as with AIDS patients without OI (p less than 0.01). In addition, the production of TNF by AM in these subjects was higher than that by the corresponding blood monocytes (p less than 0.02), suggesting a compartmentalization of this response within the lungs. In conclusion, it appears that the TNF production by AM of seropositive patients is highly related to the presence of lung OI as well as to the expression of HIV by these cells. In the context of the up-regulation of HIV expression induced by TNF in vitro, our data could suggest that the in vivo release of TNF by AM could participate in viral dissemination. Moreover, we hypothesize that the generation of activated AM refractory to any further stimulation could in turn lead to the development of additional pulmonary infections.

Published
1991

24. Veritas ipsa promissum

Author

Larcher, R., primary, Andrieu, J.-M., additional, Ramdani, M., additional, Passebois, L., additional, Favier, L., additional, Oziol, E., additional, and Duffau, P., additional

Published
2013
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36. Corrected area under prostate-specific antigen (PSA) curve and PSA half-time dynamics during chemotherapy. A new prognostic classification for hormone-refractory prostate cancer (HRPC) patients

Author

Beuzeboc, P., primary, Banu, E., additional, Goubely Brewer, Y., additional, Banu, A., additional, Zerbib, M., additional, Flam, T., additional, Peyromaure, M., additional, Scotte, F., additional, Andrieu, J. M., additional, and Oudard, S., additional

Published
2005
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45. Outpatient treatment with subcutaneous interleukin-2 and interferon alfa administration in combination with fluorouracil in patients with metastatic renal cell carcinoma: results of a sequential nonrandomized phase II study. Subcutaneous Administration Propeukin Program Cooperative Group.

Author

Tourani, J M, primary, Pfister, C, additional, Berdah, J F, additional, Benhammouda, A, additional, Salze, P, additional, Monnier, A, additional, Paule, B, additional, Guillet, P, additional, Chretien, Y, additional, Brewer, Y, additional, Di Palma, M, additional, Untereiner, M, additional, Malaurie, E, additional, Tadrist, Z, additional, Pavlovitch, J M, additional, Hauteville, D, additional, Mejean, A, additional, Azagury, M, additional, Mayeur, D, additional, Lucas, V, additional, Krakowski, I, additional, Larregain-Fournier, D, additional, Abourachid, H, additional, Andrieu, J M, additional, and Chastang, C, additional

Published
1998
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46. Ten-year results of a strategy combining three cycles of ABVD and high-dose extended irradiation for treating Hodgkin’s disease at advanced stages

Author

Andrieu, J.-M., primary, Jais, J.-P., additional, Colonna, P., additional, Desablens, B., additional, Brière, J., additional, François, S., additional, Harousseau, J.-L., additional, Casassus, P., additional, Lemevel, A., additional, Le Prisé, P.-Y., additional, Ghandour, C., additional, Guilhot, F., additional, and Lejeune, F., additional

Published
1998
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47. Mediastinal tumor size and response to chemotherapy are the only prognostic factors in supradiaphragmatic Hodgkin's disease treated by ABVD plus radiotherapy: ten-year results of the Paris-Ouest-France 81/12 trial, including 262 patients.

Author

Colonna, P, primary, Jais, J P, additional, Desablens, B, additional, Harousseau, J L, additional, Brière, J, additional, Boasson, M, additional, Lemevel, A, additional, Casassus, P, additional, Le Prisé, P Y, additional, Guilhot, F, additional, Ghandour, C, additional, Lejeune, F, additional, and Andrieu, J M, additional

Published
1996
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