Your search keyword '"Gil-Cruz, Cristina"' showing total 6 results

1. Antibodies as biomarker candidates for response and survival to checkpoint inhibitors in melanoma patients

Author

Fässler, Mirjam, Diem, Stefan, Mangana, Joanna, Hasan Ali, Omar, Berner, Fiamma, Bomze, David, Ring, Sandra, Niederer, Rebekka, Del Carmen Gil Cruz, Cristina, Pérez Shibayama, Christian Ivan, Krolik, Michal, Siano, Marco, Joerger, Markus, Recher, Mike, Risch, Lorenz, Güsewell, Sabine, Risch, Martin, Speiser, Daniel E, Ludewig, Burkhard, Levesque, Mitchell P, Dummer, Reinhard, Flatz, Lukas, University of Zurich, and Flatz, Lukas

Subjects

Male, Antibodies, Neoplasm, 610 Medicine & health, Metastatic melanoma, Antibodies, Monoclonal, Humanized, lcsh:RC254-282, Antibodies, TRP2, TRP1, Antineoplastic Agents, Immunological, Humans, NY-ESO-1, 1306 Cancer Research, Immune response, Melanoma, Aged, Aged, 80 and over, 2403 Immunology, 10177 Dermatology Clinic, Biomarker, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Ipilimumab, 3004 Pharmacology, Nivolumab, gp100, 1313 Molecular Medicine, Immunoglobulin G, 2723 Immunology and Allergy, Melanocyte differentiation antigens, MART1, 2730 Oncology, Antibodies, Monoclonal, Humanized/therapeutic use, Antibodies, Neoplasm/blood, Antineoplastic Agents, Immunological/therapeutic use, Biomarkers, Female, Immunoglobulin G/blood, Ipilimumab/therapeutic use, Melanoma/blood, Melanoma/drug therapy, Melanoma/immunology, Nivolumab/therapeutic use, Cancer/testis antigens, Checkpoint inhibitors, Research Article

Abstract

Background Long-term survival of stage IV melanoma patients has improved significantly with the development of immune checkpoint inhibitors (CIs). Reliable biomarkers to predict response and clinical outcome are needed. Methods We investigated the role of melanoma-associated antibodies as predictive markers for CI therapy in two independent cohorts. In cohort 1, a prospective study, we measured specific antibodies before treatment, after one week and after six to nine weeks of treatment. Cohort 2 consisted of serum samples prior to CI therapy initiation. ELISA assays were performed to quantify specific IgG directed against melanocyte differentiation antigens tyrosinase-related proteins 1 and 2 (TRP1/TYRP1 and TRP2/TYRP2), glycoprotein 100 (gp100), MelanA/MART1, and the cancer-testis antigen NY-ESO-1. Response was defined as either complete or partial remission on CT scan according to RECIST 1.1. Results In cohort 1, baseline levels of these antibodies were higher in the responder group, although statistical significance was only reached for NY-ESO-1 (p = 0.007). In cohort 2, significantly higher antibody baseline levels for MelanA/MART1 (p = 0.003) and gp100 (p = 0.029) were found. After pooling the results from both cohorts, higher levels of MelanA/MART1 (p = 0.013), TRP1/TYRP1 (p = 0.048), TRP2/TYRP2 (p = 0.047) and NY-ESO-1 (p = 0.005) specific antibodies at baseline were independently associated with response. Conclusions Melanoma-associated antibodies may be candidate biomarkers for response and survival in metastatic melanoma patients being treated with CIs. These markers may be used to complement patient assessment, in combination with PD-L1 status, tumor-infiltrating lymphocytes and tumor mutational burden, with the aim to predict outcome of CI treatment in patients with metastatic melanoma. Trial registration Ethikkommission Ostschweiz, EKOS 16/079 https://ongoingprojects.swissethics.ch/runningProjects_list.php?q=%28BASECID~contains~2016-00998%29&orderby=dBASECID. Electronic supplementary material The online version of this article (10.1186/s40425-019-0523-2) contains supplementary material, which is available to authorized users.

Published

2019

2. Evolution of Salmonella Typhi outer membrane protein-specific T and B cell responses in humans following oral Ty21a vaccination: A randomized clinical trial.

Author

Carreño, Juan Manuel, Perez-Shibayama, Christian, Gil-Cruz, Cristina, Lopez-Macias, Constantino, Vernazza, Pietro, Ludewig, Burkhard, and Albrich, Werner C.

Subjects

SALMONELLA typhi, BACTERIAL outer membrane proteins, T cells, B cells, ORAL drug administration, SALMONELLA diseases, VACCINATION

Abstract

Vaccination against complex pathogens such as typhoidal and non-typhoidal Salmonella requires the concerted action of different immune effector mechanisms. Outer membrane proteins (Omps) of Salmonella Typhi are potent immunogens, which elicit long-lasting and protective immunity. Here, we followed the evolution of S. Typhi OmpC and F-specific T and B cell responses in healthy volunteers after vaccination with the vaccine strain Ty21a. To follow humoral and cellular immune responses, pre- and post-vaccination samples (PBMC, serum and stool) collected from 15 vaccinated and 5 non-vaccinated individuals. Immunoglobulin levels were assessed in peripheral blood by enzyme-linked immunosorbent assay. B cell and T cell activation were analyzed by flow cytometry. We observed a significant increase of circulating antibody-secreting cells and maximal Omp-specific serum IgG titers at day 25 post vaccination, while IgA titers in stool peaked at day 60. Likewise, Omp-specific CD4+ T cells in peripheral blood showed the highest expansion at day 60 post vaccination, concomitant with a significant increase in IFN-γ and TNFα production. These results indicate that S. Typhi Omp-specific B cell responses and polyfunctional CD4+ T cell responses evolve over a period of at least two months after application of the live attenuated vaccine. Moreover, these findings underscore the potential of S. Typhi Omps as subunit vaccine components. Trial registration: [ABSTRACT FROM AUTHOR]

Published

2017

3. Early endonuclease-mediated evasion of RNA sensing ensures efficient coronavirus replication.

Author

Kindler, Eveline, Gil-Cruz, Cristina, Spanier, Julia, Li, Yize, Wilhelm, Jochen, Rabouw, Huib H., Züst, Roland, Hwang, Mihyun, V’kovski, Philip, Stalder, Hanspeter, Marti, Sabrina, Habjan, Matthias, Cervantes-Barragan, Luisa, Elliot, Ruth, Karl, Nadja, Gaughan, Christina, van Kuppeveld, Frank J. M., Silverman, Robert H., Keller, Markus, and Ludewig, Burkhard

Subjects

*ENDONUCLEASES, *CORONAVIRUSES, *RNA virus infections, *SARS disease, *QUORUM sensing, *TYPE I interferons, *IMMUNE response

Abstract

Coronaviruses are of veterinary and medical importance and include highly pathogenic zoonotic viruses, such as SARS-CoV and MERS-CoV. They are known to efficiently evade early innate immune responses, manifesting in almost negligible expression of type-I interferons (IFN-I). This evasion strategy suggests an evolutionary conserved viral function that has evolved to prevent RNA-based sensing of infection in vertebrate hosts. Here we show that the coronavirus endonuclease (EndoU) activity is key to prevent early induction of double-stranded RNA (dsRNA) host cell responses. Replication of EndoU-deficient coronaviruses is greatly attenuated in vivo and severely restricted in primary cells even during the early phase of the infection. In macrophages we found immediate induction of IFN-I expression and RNase L-mediated breakdown of ribosomal RNA. Accordingly, EndoU-deficient viruses can retain replication only in cells that are deficient in IFN-I expression or sensing, and in cells lacking both RNase L and PKR. Collectively our results demonstrate that the coronavirus EndoU efficiently prevents simultaneous activation of host cell dsRNA sensors, such as Mda5, OAS and PKR. The localization of the EndoU activity at the site of viral RNA synthesis–within the replicase complex—suggests that coronaviruses have evolved a viral RNA decay pathway to evade early innate and intrinsic antiviral host cell responses. [ABSTRACT FROM AUTHOR]

Published

2017

4. HDAC1 Controls CD8+ T Cell Homeostasis and Antiviral Response.

Author

Tschismarov, Roland, Firner, Sonja, Gil-Cruz, Cristina, Göschl, Lisa, Boucheron, Nicole, Steiner, Günter, Matthias, Patrick, Seiser, Christian, Ludewig, Burkhard, and Ellmeier, Wilfried

Subjects

T cells, HOMEOSTASIS, ANTIVIRAL agents, ACETYLATION, LYSINE, CELLULAR control mechanisms

Abstract

Reversible lysine acetylation plays an important role in the regulation of T cell responses. HDAC1 has been shown to control peripheral T helper cells, however the role of HDAC1 in CD8+ T cell function remains elusive. By using conditional gene targeting approaches, we show that LckCre-mediated deletion of HDAC1 led to reduced numbers of thymocytes as well as peripheral T cells, and to an increased fraction of CD8+CD4– cells within the CD3/TCRβlo population, indicating that HDAC1 is essential for the efficient progression of immature CD8+CD4– cells to the DP stage. Moreover, CD44hi effector CD8+ T cells were enhanced in mice with a T cell-specific deletion of HDAC1 under homeostatic conditions and HDAC1-deficient CD44hi CD8+ T cells produced more IFNγ upon ex vivo PMA/ionomycin stimulation in comparison to wild-type cells. Naïve (CD44l°CD62L+) HDAC1-null CD8+ T cells displayed a normal proliferative response, produced similar amounts of IL-2 and TNFα, slightly enhanced amounts of IFNγ, and their in vivo cytotoxicity was normal in the absence of HDAC1. However, T cell-specific loss of HDAC1 led to a reduced anti-viral CD8+ T cell response upon LCMV infection and impaired expansion of virus-specific CD8+ T cells. Taken together, our data indicate that HDAC1 is required for the efficient generation of thymocytes and peripheral T cells, for proper CD8+ T cell homeostasis and for an efficient in vivo expansion and activation of CD8+ T cells in response to LCMV infection. [ABSTRACT FROM AUTHOR]

Published

2014

5. Sequestration by IFIT1 Impairs Translation of 2′O-unmethylated Capped RNA.

Author

Habjan, Matthias, Hubel, Philipp, Lacerda, Livia, Benda, Christian, Holze, Cathleen, Eberl, Christian H., Mann, Angelika, Kindler, Eveline, Gil-Cruz, Cristina, Ziebuhr, John, Thiel, Volker, and Pichlmair, Andreas

Subjects

SEQUESTRATION (Chemistry), RNA, RNA methylation, INTERFERONS, MASS spectrometry, STABLE isotopes, METHYLTRANSFERASES

Abstract

Viruses that generate capped RNA lacking 2′O methylation on the first ribose are severely affected by the antiviral activity of Type I interferons. We used proteome-wide affinity purification coupled to mass spectrometry to identify human and mouse proteins specifically binding to capped RNA with different methylation states. This analysis, complemented with functional validation experiments, revealed that IFIT1 is the sole interferon-induced protein displaying higher affinity for unmethylated than for methylated capped RNA. IFIT1 tethers a species-specific protein complex consisting of other IFITs to RNA. Pulsed stable isotope labelling with amino acids in cell culture coupled to mass spectrometry as well as in vitro competition assays indicate that IFIT1 sequesters 2′O-unmethylated capped RNA and thereby impairs binding of eukaryotic translation initiation factors to 2′O-unmethylated RNA template, which results in inhibition of translation. The specificity of IFIT1 for 2′O-unmethylated RNA serves as potent antiviral mechanism against viruses lacking 2′O-methyltransferase activity and at the same time allows unperturbed progression of the antiviral program in infected cells. [ABSTRACT FROM AUTHOR]

Published

2013

6. Dendritic Cell-Specific Delivery of Flt3L by Coronavirus Vectors Secures Induction of Therapeutic Antitumor Immunity.

Author

Perez-Shibayama, Christian, Gil-Cruz, Cristina, Nussbacher, Monika, Allgäuer, Eva, Cervantes-Barragan, Luisa, Züst, Roland, and Ludewig, Burkhard

Subjects

*DENDRITIC cells, *ANTINEOPLASTIC agents, *CORONAVIRUSES, *DRUG delivery systems, *CANCER vaccines, *LYMPHOCYTES, *GREEN fluorescent protein

Abstract

Efficacy of antitumor vaccination depends to a large extent on antigen targeting to dendritic cells (DCs). Here, we assessed antitumor immunity induced by attenuated coronavirus vectors which exclusively target DCs in vivo and express either lymphocyte- or DC-activating cytokines in combination with a GFP-tagged model antigen. Tracking of in vivo transduced DCs revealed that vectors encoding for Fms-like tyrosine kinase 3 ligand (Flt3L) exhibited a higher capacity to induce DC maturation compared to vectors delivering IL-2 or IL-15. Moreover, Flt3L vectors more efficiently induced tumor-specific CD8+ T cells, expanded the epitope repertoire, and provided both prophylactic and therapeutic tumor immunity. In contrast, IL-2- or IL-15-encoding vectors showed a substantially lower efficacy in CD8+ T cell priming and failed to protect the host once tumors had been established. Thus, specific in vivo targeting of DCs with coronavirus vectors in conjunction with appropriate conditioning of the microenvironment through Flt3L represents an efficient strategy for the generation of therapeutic antitumor immunity. [ABSTRACT FROM AUTHOR]

Published

2013