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1. Reinstalling immune regulatory tryptophan catabolism in juvenile diabetes via interleukin 6 receptor blockade

Author

Mondanelli, G., Orabona, C., Pallotta, Mt, Albini, E., Volpi, C., and Grohmann, U.

Subjects
Immunology, Immunology and Allergy
Abstract

Indoleamine 2,3-dioxygenase 1 (IDO1) is a potent immunoregulatory enzyme that catalyses the degradation of the essential amino acid tryptophan (Trp) along the kynurenines pathway. Significant changes in systemic Trp catabolism have been reported in many diseases, including cancer and autoimmunity. In female nonobese (NOD) mice, IDO1 expression and hence immune tolerance to pancreatic b-cell autoantigens are defective in conventional dendritic cells stimulated with IFN-γ, the main IDO1 inducer. Although the evidences in NOD mice suggest that IDO1 function is impaired, the existence of the IDO1 defect in human T1D (type 1 diabetes) has not been proven yet. Here we monitored the IDO1 expression and activity in peripheral blood mononuclear cells (PBMCs) of children with T1D as compare to age-matched control subject, in response to IFN- γ. Results from kynurenines assay and Western blot analysis demonstrate that the majority of patients with T1D is characterized by defective Trp catabolism. Moreover, our data indicated that this defect is mainly imputable to a SOCS3-mediated, dysregulated IL-6 signaling that would favor IDO1 proteasomal degradation in inflammatory environments, i.e. dominated by IFN-γ. To confirm this, we measured IDO1 expression and activity in PBMCs co-incubated with IFN-γ and Tocilizumab (TCZ), a licensed IL-6 receptor blocker. Results showed that TCZ is able to restore normal levels of IDO1 catalytic activity in response to IFN-γ in approximately 30% of the examined T1D population. Besides further confirming the heterogeneity of the disease, our data indicate the existence of a subset of individuals with T1D who may gain clinical benefit in restoring immunoregulatory mechanisms by treatment with tocilizumab.

Published
2016
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3. Dacarbazine-induced immunogenicity of a murine leukemia is attenuated in cells transfected with mutated K-ras gene

Author

Testorelli, C., Bussini, S., Filippi, R., Marelli, O., Orlando, L., Greiner, J. W., Grohmann, U., Tentori, L., Giuliani, A., Bonmassar, E., GRAZIA GRAZIANI, Testorelli, C, Bussini, S, DE FILIPPI, Rosaria, Marelli, O, Orlando, L, Greiner, Jw, Grohmann, U, Tentori, L, Giuliani, A, Bonmassar, E, and Graziani, G.

Subjects
Mice, Inbred BALB C, triazenes, Histocompatibility Antigens Class I, leukemia, Settore BIO/14, Antineoplastic Agents, mutated oncogene, immunogenicity, Transfection, Dacarbazine, Mice, Genes, ras, Mice, Inbred DBA, K-ras, xenogenization, Animals, Leukemia L5178
Abstract

Strong immunogenicity is induced by antitumor triazene compounds in tumor cells through a mutagenic mechanism. A highly immunogenicDclone, isolated from a dacarbazine-treated L5178Y leukemia of DBA/2 mice, was transfected with K-ras mutated at codon 12 (i.e. ras(m12)). This transfected clone presents at least 2 mutations, one concerning K-ras gene, and the other affecting an unrelated gene, responsible for the generation of a highly immunogenic, MHC class I restricted non-self peptide. The results indicate that cells ofDclone transfected with ras(m12) were less immunogenic than cells of the same origin transfected with the vector alone. Moreover, ras(m12)-transfected cells showed lower levels of H-2K(d) gene expression with respect to those detectable in control cells. In addition, in vivo and in vitro sensitization againstDclone carrying mutated ras did not result in a strong cytotoxic T lymphocyte response against ras(m12)-transfected non immunogenic L5178y target cells. These preliminary results suggest that K-ras mutation could down-regulate the level of tumor immunogenicity, possibly acquired through a mutagenic process affecting other unrelated genes.

4. IL-12 Is Both Required and Sufficient for Initiating T Cell Reactivity to a Class I-Restricted Tumor Peptide (P815AB) Following Transfer of P815AB-Pulsed Dendritic Cells

Author

Bianchi, R., Grohmann, U., Belladonna, M. L., Silla, S., Fallarino, F., Emira Ayroldi, Fioretti, M. C., and Puccetti, P.

Subjects
IL-12, tumor vaccines, Immunology, Immunology and Allergy, tumor peptide, dendritic cells
Abstract

Delayed-type hypersensitivity responses, mediated by CD8+ cells and detected by skin test assay, occur in sensitized mice in response to challenge with a class I-restricted synthetic peptide related to a poorly immunogenic tumor rejection Ag, P815AB, of murine mastocytoma cells. Efficient priming for this response, which requires functional CD4+ cells and production of IFN-gamma in the host, is achieved by transfer of dendritic cells (DC) pulsed in vitro with a physical mixture of P815AB and T helper peptides, such as a class II-restricted synthetic peptide of tetanus toxin. We now show that the adjuvant effect of the T helper peptide was associated with the appearance of early and late IL-12 transcripts in the spleens of DC recipient mice, correlated with a late IFN-gamma response, and was negated by serologic ablation of endogenous IL-12 at the time of cell transfer. rIL-12, administered in vivo to the DC recipient mice, could substitute for the T helper peptide in initiating skin test reactivity following transfer of DC pulsed with P815AB alone, leading to Ag-specific production of IFN-gamma by CD4+ and CD8+ T cells. In vitro and in vivo cell depletion experiments suggested the following: 1) the exogenous IL-12 required both CD4+ and CD8+ cells for activity; 2) the immune response initiated by IL-12 relied on later production of IL-12 by the host; and 3) the early adjuvanticity of the exogenous IL-12 involved improved recognition of class II-restricted epitopes of this otherwise poorly immunogenic tumor peptide.

5. IL-12 acts selectively on CD8 alpha- dendritic cells to enhance presentation of a tumor peptide in vivo

Author

Grohmann U, Bianchi R, Ml, Belladonna, Carmine Vacca, Silla S, Ayroldi E, Mc, Fioretti, and Puccetti P

Subjects
Clonal Anergy, Male, Antigen Presentation, CD8 Antigens, Receptors, Interleukin-12, Dendritic Cells, Receptors, Interleukin, Interleukin-12, Recombinant Proteins, Interleukin-10, Mice, Antigens, Neoplasm, Mice, Inbred DBA, Injections, Intravenous, Animals, Hypersensitivity, Delayed, Immunization, RNA, Messenger, Oligopeptides
Abstract

Previous work has shown that a significant proportion of murine splenic dendritic cells (DC) express a high affinity receptor for IL-12, thus accounting for the adjuvanticity of the cytokine when DBA/2 mice are transferred with syngeneic DC exposed in vitro to rIL-12 and an otherwise poorly immunogenic tumor peptide. In DBA/2 mice, splenic DC consist of 90-95% CD8- and 5-10% CD8+ cells. To detect any difference in IL-12 responsiveness among phenotypically distinct DC subtypes, enriched CD8- (99% pure) and CD8+ ( approximately 80% pure) populations of DC from DBA/2 spleens were assayed for APC function in vivo following exposure to rIL-12 and tumor peptide in vitro. Unlike unfractionated DC, the CD8- fraction was capable of effective presentation of the peptide even when the cells had not been pretreated with IL-12 before peptide pulsing. The addition of as few as 3% CD8+ cells during pulsing blocked in vivo priming by the CD8- fraction. However, pretreatment of CD8- DC with IL-12 before cell mixing and peptide pulsing ablated the inhibitory effect of the CD8+ fraction. CD8-, but not CD8+, DC showed significant message expression for the beta 1 and beta 2 subunits of the IL-12 receptor. These data suggest that a minority population of CD8+ DC, which appeared to secrete IL-10 in vitro, negatively regulates the induction of T cell reactivity by peptide-loaded CD8- DC in DBA/2 mice. However, the CD8- fraction can be primed by IL-12 to overcome the inhibitory effect of the CD8+ subtype.

6. A Tumor-Associated and Self Antigen Peptide Presented by Dendritic Cells May Induce T Cell Anergy in Vivo, but IL-12 Can Prevent or Revert the Anergic State

Author

Grohmann, U., Roberta Bianchi, Ayroldi, E., Belladonna, M. L., Surace, D., Fioretti, M. C., and Puccetti, P.

Subjects
Immunology, Immunology and Allergy
Abstract

Ag-specific CD8+ cell responses, including delayed-type hypersensitivity in vivo and IFN-gamma production in vitro, are initiated by host immunization with P815AB, a self peptide bearing CTL epitopes and expressed by murine mastocytoma cells. Using P815AB-pulsed dendritic cells (DC) and monitoring class I-restricted skin test reactivity in DC-primed mice, we have previously shown that the development of a Th1-like response to P815AB requires T helper effects, such as those mediated by coimmunization with class II-restricted (helper) peptides or by the use of rIL-12. The adjuvanticity of IL-12 was suggested to involve improved recognition of class II-restricted epitopes of P815AB. In the present study, we provide evidence for the occurrence of I-A(d)-restricted epitopes in the tumor peptide. We also show that in the absence of helper peptide or rIL-12, P81 5AB not only failed to initiate CD8+ cell responses in vivo and in vitro, but resulted in a transient state of functional unresponsiveness, characterized by a profound inability of CD4+ cells to produce IL-2 in vitro. Ag-specific T cell anergy was also observed after neutralization of endogenous IL-12 at the time of priming with P815AB plus helper peptide. All of these effects were reversed by rIL-12, which was added to DC cultures and administered to the DC-recipient mice. Anergy induction may thus contribute to P81 5AB unresponsiveness in vivo. IL-12 may act to prevent or revert anergy to this tumor-associated and self peptide.

7. Autocrine IL-12 is involved in dendritic cell modulation via CD40 ligation

Author

Bianchi, R., Grohmann, U., Vacca, C., Belladonna, M. L., Fioretti, M. C., and Paolo Puccetti

Subjects
Male, Antigen Presentation, Tumor Necrosis Factor-alpha, Immunology, CD40 ligation tumor vaccines, Antibodies, Monoclonal, Ligands, Recombinant Proteins, Autocrine Communication, Interferon-gamma, Mice, Adjuvants, Immunologic, Mice, Inbred DBA, IL-12, dendritic cells, Immunology and Allergy, Animals, Interleukin-2, CD40 Antigens, Peptides, Interleukin-1
Abstract

Ligation of CD40 on dendritic cells (DC) triggers production of IL-12. Using an adoptive transfer model we have previously shown that rIL-12 acts directly on DC to enhance presentation of an otherwise poorly immunogenic tumor peptide. Using the same experimental model, we now describe a similar adjuvanticity of CD40 ligation on peptide presentation by DC. We also explore the possibility that the IL-12 resulting from CD40 ligation directly affects the APC function of DC, mediating or contributing to the adjuvant effect of CD40 ligation. CD40 engagement in vitro and rIL-12 at concentrations in the range induced by CD40 ligation were equally effective in priming DC for presentation of the tumor peptide in vivo. Remarkably, the copresence in vitro of neutralizing Ab to IL-12, but not to TNF-α, IL-1β, or IFN-γ, ablated the enhancing effect of CD40 engagement on the APC function of DC. These data suggest a major role for autocrine IL-12 in DC modulation via CD40 ligation.

8. Multiple point mutations in an endogenous retroviral gene confer high immunogenicity on a drug-treated murine tumor

Author

Grohmann, U., Paolo Puccetti, Belladonna, M. L., Fallarino, F., Bianchi, R., Binaglia, L., Sagakuchi, K., Mage, M. G., Appella, E., and Fioretti, M. C.

Subjects
Immunology, Immunology and Allergy
Abstract

Exposure in vivo of murine L5178Y lymphoma cells to cytoreductive triazene derivatives leads to the generation of immunogenic variant lines expressing new transplantation Ags recognized by CTL. In one such clonal variant (clone D), at least one subset of T cell neoepitopes are provided by proteins previously shown by serology to be products of endogenous retroviral env sequences. We report here on characterization of PCR-amplified gp70 env genes in clone D. Relative to known gp70 sequences in parental cells and in current databases, one gp70 sequence presented four distinct nucleotide changes, two of which were apparently unique to clone D DNA and cDNA upon differential hybridization analysis. Transfection experiments with the entire gp70 gene or subgenic fragments encompassing a single putative mutation showed that products of the mutated env gene or fragments may confer immunogenicity in vivo and susceptibility in vitro to lysis by clone D-primed, H-2Kd- or H-2Ld-restricted CTL. By skin test assay of mice primed with either clone D or three mutated synthetic peptides, evidence was obtained that amino acid substitutions at the relevant positions of the gp70 protein may produce immunogenic T cell epitopes and that these epitopes are expressed in vivo by clone D. These data point to the role of mutated retroviral tumor peptides as rejection Ags in histocompatible hosts.

13. Neutralization of IL-10 up-regulates nitric oxide production and protects susceptible mice from challenge with Candida albicans

Author

Luigina Romani, Puccetti P, Mencacci A, Cenci E, Spaccapelo R, Tonnetti L, Grohmann U, and Bistoni F

Subjects
CD4-Positive T-Lymphocytes, Cytotoxicity, Immunologic, Male, Molecular Sequence Data, Immunology, Gene Expression, Nitric Oxide, Candida albicans, Ifn-gamma, Interferon-gamma, Mice, Animals, Immunology and Allergy, Hypersensitivity, Delayed, RNA, Messenger, DNA Primers, Immunity, Cellular, Mice, Inbred BALB C, Base Sequence, Macrophages, Candidiasis, Interleukin-10, Mice, Inbred C57BL, Mice, Inbred DBA, Female, Interleukin-4
Abstract

In contrast to several inbred strains of mice that develop Th1-associated anticandidal protection, DBA/2 mice are highly susceptible to systemic infection with Candida albicans cells of the attenuated variant PCA-2, and fatal outcome is observed in concurrence with sustained CD4+ cell production in vitro of IL-4 and IL-10. These Th2 cytokines were previously shown to inhibit nitric oxide (NO) production and yeast killing by activated macrophage cultures. We now show that macrophages from DBA/2 mice, either intact or infected with PCA-2, have lower capacity than resistant strains to synthesize NO in response to IFN-gamma. However, when treated with anti-IL-10 Abs at the time of infection, DBA/2 mice survived challenge and displayed increased production of NO in vitro after IFN-gamma activation. Cure was associated with the onset of footpad responses and durable protection, and higher frequencies of IFN-gamma-secreting cells were found in splenic CD4+ lymphocytes that expressed lower levels of IL-4 and IL-10 mRNA. Therefore, in DBA/2 mice, IL-10 contributes significantly to the selection of a Th2 response and lethality after PCA-2 challenge. An IL-10-induced defect in the activation and/or expansion of IFN-gamma-producing Th1 cells, IL-10 suppression of yeast killing, and the relative inability of DBA/2 macrophages to produce adequate levels of candidacidal NO may all contribute to the abnormal susceptibility of these mice to candidiasis.

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