Your search keyword '"Dotti, G"' showing total 15 results

1. Bortezomib sensitizes non-small cell lung cancer to mesenchymal stromal cell-delivered inducible caspase-9-mediated cytotoxicity.

Author

Ando, M, Hoyos, V, Yagyu, S, Tao, W, Ramos, C A, Dotti, G, Brenner, M K, and Bouchier-Hayes, L

Subjects

BORTEZOMIB, CANCER treatment, NON-small-cell lung carcinoma, GENE targeting, MESENCHYME, STROMAL cells, CASPASES, CELL-mediated cytotoxicity, THERAPEUTICS

Abstract

Delivery of suicide genes to solid tumors represents a promising tumor therapy strategy. However, slow or limited killing by suicide genes and ineffective targeting of the tumor has reduced effectiveness. We have adapted a suicide system based on an inducible caspase-9 (iC9) protein that is activated using a specific chemical inducer of dimerization (CID) for adenoviral-based delivery to lung tumors via mesenchymal stromal cells (MSCs). Four independent human non-small cell lung cancer (NSCLC) cell lines were transduced with adenovirus encoding iC9, and all underwent apoptosis when iC9 was activated by adding CID. However, there was a large variation in the percentage of cell killing induced by CID across the different lines. The least responsive cell lines were sensitized to apoptosis by combined inhibition of the proteasome using bortezomib. These results were extended to an in vivo model using human NSCLC xenografts. E1A-expressing MSCs replicated Ad.iC9 and delivered the virus to lung tumors in SCID mice. Treatment with CID resulted in some reduction of tumor growth, but addition of bortezomib led to greater reduction of tumor size. The enhanced apoptosis and anti-tumor effect of combining MSC-delivered Ad.iC9, CID and bortezomib appears to be due to increased stabilization of active caspase-3, as proteasomal inhibition increased the levels of cleaved caspase-9 and caspase-3. Knockdown of X-linked inhibitor of apoptosis protein (XIAP), a caspase inhibitor that targets active caspase-3 to the proteasome, also sensitized iC9-transduced cells to CID, suggesting that blocking the proteasome counteracts XIAP to permit apoptosis. Thus, MSC-based delivery of the iC9 suicide gene to human NSCLC effectively targets lung cancer cells for elimination. Combining this therapy with bortezomib, a drug that is otherwise inactive in this disease, further enhances the anti-tumor activity of this strategy. [ABSTRACT FROM AUTHOR]

Published

2014

2. The immunogenicity of virus-derived 2A sequences in immunocompetent individuals.

Author

Arber, C, Abhyankar, H, Heslop, H E, Brenner, M K, Liu, H, Dotti, G, and Savoldo, B

Subjects

NUCLEOTIDE sequence, IMMUNOCOMPETENT cells, GENETIC engineering, T cells, IMMUNOTHERAPY, CANCER patients, GENE expression

Abstract

Genetic engineering of T cells for adoptive immunotherapy in cancer patients has shown significant promise. To ensure optimal antitumor activity and safety, the simultaneous expression of multiple genes is frequently required, and short viral-derived 2A sequences are increasingly preferred for this purpose. Concerns exist, however, that these virus-derived sequences may induce unwanted immune responses, and thus diminish persistence of the gene-modified cells after adoptive transfer. Whereas such responses were absent in immunocompromised recipients, potential immunogenicity in immunocompetent individuals remains a concern. We now address whether ex vivo T cell responses can be elicited against the most widely used 2A sequences (2A-Thosea asigna virus (TAV) or 2A-equine rhinitis virus (ERAV), specifically) in immunocompetent individuals. We used a potent ex vivo culture system previously validated to induce T cell responses even against weakly immunogenic antigens. Of the sixteen donors tested, only five released very low levels of interferon-γ in response to 2A-TAV peptide mixtures (single peptide specificity in three donors, adjacent self-antigen peptide specificity in one donor and nonspecific reactivity in one donor). None of them produced cytotoxic activity or responded to 2A-ERAV. These results suggest that exposure to viral-derived 2A sequences is unlikely to produce unwanted T cell responses in immunocompetent individuals and further supports their continued use for studies of human gene therapy. [ABSTRACT FROM AUTHOR]

Published

2013

3. Engineering CD19-specific T lymphocytes with interleukin-15 and a suicide gene to enhance their anti-lymphoma/leukemia effects and safety.

Author

Hoyos, V., Savoldo, B., Quintarelli, C., Mahendravada, A., Zhang, M., Vera, J., Heslop, H. E., Rooney, C. M., Brenner, M. K., and Dotti, G.

Subjects

T cells, CELL death, B cells, LYMPHOMAS, T-cell lymphoma, ANIMAL experimentation, ANTIGENS, CELLULAR immunity, GENES, IMMUNOLOGY technique, IMMUNOPHENOTYPING, INTERLEUKINS, LEUKEMIA, MICE, PROTEINS, RESEARCH funding, PREVENTION

Abstract

T lymphocytes expressing a chimeric antigen receptor (CAR) targeting the CD19 antigen (CAR.19) may be of value for the therapy of B-cell malignancies. Because the in vivo survival, expansion and anti-lymphoma activity of CAR.19(+) T cells remain suboptimal even when the CAR contains a CD28 costimulatory endodomain, we generated a novel construct that also incorporates the interleukin-15 (IL-15) gene and an inducible caspase-9-based suicide gene (iC9/CAR.19/IL-15). We found that compared with CAR.19(+) T cells, iC9/CAR.19/IL-15(+) T cells had: (1) greater numeric expansion upon antigen stimulation (10-fold greater expansion in vitro, and 3- to 15-fold greater expansion in vivo) and reduced cell death rate (Annexin-V(+)/7-AAD(+) cells 10+/-6% for iC9/CAR.19/IL-15(+) T cells and 32+/-19% for CAR.19(+) T cells); (2) reduced expression of the programmed death 1 (PD-1) receptor upon antigen stimulation (PD-1(+) cells <15% for iC9/CAR.19/IL-15(+) T cells versus >40% for CAR.19(+) T cells); and (3) improved antitumor effects in vivo (from 4.7- to 5.4-fold reduced tumor growth). In addition, iC9/CAR.19/IL-15(+) T cells were efficiently eliminated upon pharmacologic activation of the suicide gene. In summary, this strategy safely increases the anti-lymphoma/leukemia effects of CAR.19-redirected T lymphocytes and may be a useful approach for treatment of patients with B-cell malignancies. [ABSTRACT FROM AUTHOR]

Published

2010

4. Selective elimination of a chemoresistant side population of B-CLL cells by cytotoxic T lymphocytes in subjects receiving an autologous hCD40L/IL-2 tumor vaccine.

Author

Foster, A E, Okur, F V, Biagi, E, Lu, A, Dotti, G, Yvon, E, Savoldo, B, Carrum, G, Goodell, M A, Heslop, H E, and Brenner, M K

Subjects

CANCER cells, TISSUES, CHRONIC lymphocytic leukemia, T cells, B cells, ANTIGENS, IMMUNIZATION, ANTIGEN analysis, CHRONIC lymphocytic leukemia treatment, ANTIMETABOLITES, ANTIVIRAL agents, CARRIER proteins, DRUG resistance in cancer cells, GLYCOPROTEINS, PROTEINS, RESEARCH funding, CANCER vaccines, PHARMACODYNAMICS

Abstract

Side-population (SP) analysis identifies precursor cells in normal and malignant tissues. Cells with this phenotype have increased resistance to many cytotoxic agents, and may represent a primary drug-resistant population in malignant diseases. To discover whether drug-resistant malignant SP cells are nonetheless sensitive to immune-mediated killing, we first established the presence of a malignant CD5(+)CD19(+) SP subset in the blood of 18/21 subjects with B-cell chronic lymphocytic leukemia (B-CLL). We examined the fate of these cells in six of these individuals who received autologous human CD40 ligand and interleukin-2 (hCD40L/IL-2) gene-modified tumor cells as part of a tumor vaccine study. Vaccinated patients showed an increase in B-CLL-reactive T cells followed by a corresponding decline in circulating CD5(+)CD19(+) SP cells. T-cell lines and clones generated from vaccinated patients specifically recognized B-CLL SP tumor cells. Elimination of SP cells is likely triggered by their increased expression of target antigens, such as receptor for hyaluronan-mediated motility (RHAMM), after stimulation of the malignant cells by hCD40L, as CD8(+) RHAMM-specific T cells could be detected in the peripheral blood of immunized patients and were associated with the decline in B-CLL SP cells. Hence, malignant B cells with a primary drug-resistant phenotype can be targeted by T- cell-mediated effector activity after immunization of human subjects. [ABSTRACT FROM AUTHOR]

Published

2010

5. Addition of the CD28 signaling domain to chimeric T-cell receptors enhances chimeric T-cell resistance to T regulatory cells.

Author

Loskog, A., Giandomenico, V., Rossig, C., Pule, M., Dotti, G., and Brenner, M. K.

Subjects

T cells, CANCER cells, LYMPHOCYTES, ANTIGEN-antibody reactions, CANCER patients, ANTIGENS

Abstract

T cells can be engineered to target tumor cells by transduction of tumor-specific chimeric receptors, consisting of an extracellular antigen-binding domain and an intracellular signaling domain. However, the peripheral blood of cancer patients frequently contains an increased number of T regulatory cells, which appear to inhibit immune reactivity. We have investigated the effects of T regulatory cells on chimeric T cells specific for the B-cell antigen CD19, as B-cell malignancies are attractive targets for chimeric T-cell therapy. When a CD19 single-chain Fv antibody was coupled to the CD3 zeta (ζ) chain, there was sharply reduced activity on exposure to T regulatory cells, measured by CD19+ target-induced proliferation and cytotoxicity. By contrast, expression in T cells of a chimeric receptor consisting of the intracellular portion of the CD28 molecule fused to the ζ-chain and CD19 single-chain Fv not only produced a higher proliferative response and an increased nuclear factor κB activation but also sustained these activities in the presence of T regulatory cells. These effects are seen whether the chimeric T cells are derived from normal donors or from patients with B-cell chronic lymphocytic leukemia, indicating the potential for clinical application in B cell malignancies.Leukemia (2006) 20, 1819–1828. doi:10.1038/sj.leu.2404366; published online 17 August 2006 [ABSTRACT FROM AUTHOR]

Published

2006

6. Current status of genetic modification of T cells for cancer treatment.

Author

Dotti, G. and Heslop, H. E.

Subjects

GENETICS, HEMATOLOGY, VIRUS diseases, T cells, GENES, IMMUNE response

Abstract

Clinical studies of adoptive immunotherapy with T cells have shown activity directed at hematologic and solid malignancies and viral infections. Genetic modification of infused T cells offers the prospect of improving such therapies and has already been used to track infused T cells, insert suicide genes and redirect the immune response towards specific Ag. Pre-clinical studies are evaluating novel approaches to genetically modify T cells to confer resistance to tumor evasion mechanisms. There is also increasing interest in developing suicide gene strategies as a failsafe mechanism to eradicate genetically modified cells should adverse effects occur. [ABSTRACT FROM AUTHOR]

Published

2005

7. Cancer vaccines: dream, reality, or nightmare?

Author

Biagi, E., Rousseau, R. F., Yvon, E., Vigouroux, S., Dotti, G., and Brenner, M. K.

Abstract

Over the past 30 years, a multidisciplinary approach com-bining surgery, chemotherapy, and radiation has led to a dramatic improvement in survival for patients affected by malignant diseases. Cellular therapies, such as stem cell transplantation, have also made a significant contribution. Nonetheless, many patients are still resistant to standard therapies, which also have high and often unacceptable acute and chronic organ toxicity, with an increased risk for secondary malignancies. Therefore new strategies are needed to improve overall survival and decrease treatment-asso-ciated morbidity. Immunotherapy represents one of the most appealing of these approaches, and active immunization in particular has proved to be amongst the most important of these new cellular strategies because of its ability to stimulate the immune system to actively recognize and kill the malignant cells. Identification of antigens expressed on tumor cells (Table 1), together with a better understanding of the molecular and cellular mechanisms involved in the immune response against cancer, have given investigators tools to manipulate the immune system to induce an efficient immune response in the tumor-bearing host [1-5]. The present review describes the approaches used in cancer vaccination that are intended not only to optimize antitu-mor immunity, but also to overcome tumor immune escape. Examples of how these approaches are being applied clinically are also given. [ABSTRACT FROM AUTHOR]

Published

2002

8. Molecular profile of Epstein-Barr virus infection in HHV-8-positive primary effusion lymphoma.

Author

Fassone, L, Bhatia, K, Gutierrez, M, Capello, D, Gloghini, A, Dolcetti, R, Vivenza, D, Ascoli, V, Coco, F Lo, Pagani, L, Dotti, G, Rambaldi, A, Raphael, M, Tirelli, U, Saglio, G, Magrath, I T, Carbone, A, Gaidano, G, and Lo Coco, F

Subjects

HERPESVIRUS diseases, EPSTEIN-Barr virus

Abstract

Primary effusion lymphoma (PEL) selectively involves the serous body cavities, occurs predominantly in immunodeficient patients and is infected consistently by human herpesvirus type-8. PEL is also frequently infected by Epstein-Barr virus (EBV). The precise pathogenetic role of EBV coinfection in PEL is not fully understood. The lymphoma fails to express the EBV transforming proteins EBNA-2 and LMP-1, whereas it expresses EBNA-1 (latency I phenotype). Some studies have hypothesized that other EBV-positive lymphomas expressing the latency I phenotype may associate with specific molecular variants of EBNA-1, although this issue has not been addressed in PEL. On this basis, this study is aimed at a detailed molecular characterization of EBV in PEL. Fifteen EBV positive PEL (12 AIDS-related, one post-transplant, two arising in immunocompetent hosts) were subjected to molecular characterization of the viral genes EBNA-1 and LMP-1, as well as definition of EBV type-1/type-2. The EBNA-1 gene displayed a high degree of heterogeneity in different cases of PEL, with seven distinct recognizable variants and subvariants. A wild-type LMP-1 gene was detected in 10/15 cases, whereas in 5/15 cases the LMP-1 gene harbored a deletion spanning codons 346-355. EBV type-1 occurred in 11/15 PEL whereas EBV type-2 occurred in 4/15 cases. Despite a high degree of genetic variability of the virus in different PEL cases, each single PEL harbored only one EBV variant, consistent with monoclonality of infection and suggesting that infection preceded clonal expansion. Overall, our results indicate that: (1) individual PEL cases consistently harbor a single EBV strain; (2) EBNA-1 displays a high degree of heterogeneity in different PEL cases; (3) no specific EBV genotype preferentially associates with PEL. [ABSTRACT FROM AUTHOR]

Published

2000

9. Macrolide resistance in group A streptococci.

Author

Savoia, D., Avanzini, C., Bosio, K., Volpe, G., Carpi, D., Dotti, G., and Zucca, M.

Abstract

Two hundred and twenty one Streptococcus pyogenes isolates collected from throat swabs of untreated children with uncomplicated pharyngotonsillitis living in two centres situated in the north of Italy were tested to evaluate their macrolide resistance phenotype. Isolates were also typed for T protein and assayed for opacity factor (OF) and protease production. Resistance to macrolides was found to be similar in the two centres. Fifty-one point two per cent of Torino strains and 43.5% of Pinerolo strains were not inhibited by erythromycin. Resistant strains belonged to one of three phenotypes: CR, constitutive resistance (37.9 and 42.5% in Torino and Pinerolo, respectively); IR, inducible resistance (40.9 and 17. 5%); NR, new resistance phenotype (21.2 and 40%). All the resistant and some of the susceptible strains were analysed by pulsed-field gel electrophoresis and genomic patterns were defined on the basis of band size and number. Five DNA profiles were found among erythromycin-resistant strains: three patterns characterized the NR resistance phenotype and one each the IR and CR phenotypes. The distribution of resistant strains according to their genomic patterns appears to be related to the resistance phenotype and only in some cases to the T serotype of bacteria. We conclude that the S. pyogenes strains analysed are genetically heterogeneous and therefore the high rate of erythromycin resistance observed is not caused by the spread of a single clone nor is it related to a particular serotype. [ABSTRACT FROM AUTHOR]

Published

2000

10. Standardized RT-PCR analysis of fusion gene transcripts from chromosome aberrations in acute leukemia for detection of minimal residual disease.

Author

van Dongen, J J M, Macintyre, E A, Gabert, J A, Delabesse, E, Rossi, V, Saglio, G, Gottardi, E, Rambaldi, A, Dotti, G, Griesinger, F, Parreira, A, Gameiro, P, Diáz, M González, Malec, M, Langerak, A W, San Miguel, J F, and Biondi, A

Subjects

LEUKEMIA, THERAPEUTICS

Abstract

Prospective studies on the detection of minimal residual disease (MRD) in acute leukemia patients have shown that large-scale MRD studies are feasible and that clinically relevant MRD-based risk group classification can be achieved and can now be used for designing new treatment protocols. However, multi-center international treatment protocols with MRD-based stratification of treatment need careful standardization and quality control of the MRD techniques. This was the aim of the European BIOMED-1 Concerted Action 'Investigation of minimal residual disease in acute leukemia: international standardization and clinical evaluation' with participants of 14 laboratories in eight European countries (ES, NL, PT, IT, DE, FR, SE and AT). Standardization and quality control was performed for the three main types of MRD techniques, ie flow cytometric immunophenotyping, PCR analysis of antigen receptor genes, and RT-PCR analysis of well-defined chromosomal aberrations. This study focussed on the latter MRD technique. A total of nine well-defined chromosome aberrations with fusion gene transcripts were selected: t(1;19) with E2A-PBX1, t(4;11) with MLL-AF4, t(8;21) with AML1-ETO, t(9;22) with BCR-ABL p190 and BCR-ABL p210, t(12;21) with TEL-AML1, t(15;17) with PML-RARA, inv (16) with CBFB-MYH11, and microdeletion 1p32 with SIL-TAL1. PCR primers were designed according to predefined criteria for single PCR (external primers A &xharr; B) and nested PCR (internal primers C &xharr; D) as well as for 'shifted' PCR with a primer upstream (E59 primer) or downstream (E39 primer) of the external A &xharr; B primers. The 'shifted' E primers were designed for performing an independent PCR together with one of the internal primers for confirmation (or exclusion) of positive results. Various local RT and PCR protocols were compared and subsequently a common protocol was designed, tested and adapted, resulting in a standardized RT-PCR protocol. After initial testing (with adaptations... [ABSTRACT FROM AUTHOR]

Published

1999

11. Primary effusion lymphoma after heart transplantation: a new entity associated with human herpesvirus-8.

Author

Dotti, G, Fiocchi, R, Motta, T, Facchinetti, B, Chiodini, B, Borleri, G M, Gavazzeni, G, Barbui, T, and Rambaldi, A

Subjects

IMMUNOSUPPRESSION, EPSTEIN-Barr virus, DNA analysis, COMPARATIVE studies, GENES, HEART transplantation, HERPESVIRUSES, LYMPHOMAS, RESEARCH methodology, MEDICAL cooperation, RESEARCH, EVALUATION research

Abstract

Deep immunosuppression and Epstein-Barr virus (EBV) infection promote the emergence of lymphoproliferative disorders in patients undergoing solid organ transplantation. In the last few years a new herpesvirus, named human herpesvirus-8 (HHV-8), has been identified in Kaposi's sarcoma and primary effusion lymphoma (PEL) developing in AIDS patients. Subsequently, the same viral DNA sequences have been identified in almost all cases of Kaposi's sarcoma emerged outside HIV infection, thus suggesting their possible pathogenetic role in this tumor. Similarly, the association between HHV-8 and PEL also emerged in cases without HIV infection, even though the total number of these patients is still limited. Here, we focus on the emergence of this unusual lymphoma in patients undergoing solid organ transplant and underline once again its association with the HHV-8. Moreover, despite the characteristic local growth of this peculiar type of lymphoma, we demonstrate at the molecular level, an early neoplastic spread to the bone marrow suggesting the need to investigate in more detail the origin of the disease, as well as the molecular mechanisms controlling its systemic dissemination. [ABSTRACT FROM AUTHOR]

Published

1999

12. Reverse transcription polymerase chain reaction is a reliable assay for detecting leukemic colonies generated by chronic myelogenous leukemia cells.

Author

Savoldo, B, Sammarelli, G, Dotti, G, Garau, D, Regazzi, E, Cilloni, D, Tabilio, A, Rizzoli, V, and Carlo-Stella, C

Subjects

KARYOTYPES, REVERSE transcriptase, POLYMERASE chain reaction

Abstract

Single-colony karyotyping (SCK) and reverse-transcription polymerase chain reaction (RT-PCR) are two increasingly used techniques for the quantification of leukemic colonies generated by chronic myelogenous leukemia (CML) cell fractions purged or selected in vitro. Recently, the existence of Philadelphia (Ph) chromosome positive progenitors with a silent BCR-ABL gene has been reported, thus raising concerns on the use of RT-PCR for detecting BCR-ABL positive progenitors. In order to investigate this issue further, colonies (n = 204) generated by mononuclear (MNC) or CD34+ CML cells were individually harvested, divided into two aliquots and analyzed both at the cytogenetic level to detect the Ph chromosome, and the molecular level to detect BCR-ABL transcripts. The mean (+/- s.d.) percentages of colonies analyzable by either SCK or RT-PCR were 74 +/- 16% and 86 +/- 16%, respectively. A significant percentage of colonies (67 +/- 19%) could be successfully analyzed by both SCK and RT-PCR. Although the majority of these colonies (97 +/- 5%) were Ph-positive and BCR-ABL-positive, a negligible percentage (4%) of progenitors were Ph-positive but BCR-ABL-negative. In order to test the influence of colony size on the outcome of molecular analysis, the efficiency of our RT-PCR assay in detecting BCR-ABL transcripts was investigated by means of experiments in which the number of cells used to start RNA extraction was serially reduced. These experiments showed that at least 150 cells were necessary to achieve a reproducible amplification of BCR-ABL transcripts. By correlating the size of harvested colonies with the outcome of molecular analysis, it was evident that BCR-ABL-negative but Ph-positive colonies represented false negative results occurring when a number of leukemic cells below the detection limit of our RT-PCR assay was analyzed. In conclusion, our data demonstrate that individual CML colonies grown in semisolid culture assays can be indifferently analyzed by SCK or RT-PCR, and support an extensive use of a carefully standardized RT-PCR assay to estimate the leukemic burden within samples which have been purged and selected in vitro. [ABSTRACT FROM AUTHOR]

Published

1998

13. PET imaging of T cells derived from umbilical cord blood.

Author

Singh, H., Najjar, A. M., Olivares, S., Nishii, R., Mukhopadhyay, U., Alauddin, M., Manuri, P. R., Huls, H., Lee, D. A., Dotti, G., Bollard, C., Simmons, P. J., Shpall, E. J., Champlin, R. E., Gelovani, J. G., and Cooper, L. J. N.

Subjects

LETTERS to the editor, POSITRON emission tomography, AMINOGLYCOSIDES, ANIMAL experimentation, CELL physiology, CORD blood, GENES, HEMATOPOIETIC stem cell transplantation, MICE, NUCLEOSIDES, OXIDOREDUCTASES, RADIOPHARMACEUTICALS, RECOMBINANT proteins, RESEARCH funding, T cells, TRANSFERASES, CARBOCYCLIC acids, TRANSPLANTATION of organs, tissues, etc.

Abstract

A letter to the editor is presented about a study which demonstrated the use of hygromycin phosphotransferase thymidine kinase (HyTK) fusing gene for positron emission tomography (PET) using T cells from umbilical cord blood.

Published

2009

14. CD30‐CHIMERIC ANTIGEN RECEPTOR (CAR) T CELLS FOR THERAPY OF HODGKIN LYMPHOMA (HL).

Author

Ramos, C.A., Torrano, V., Bilgi, M., Gerken, C., Dakhova, O., Mei, Z., Wu, M., Grilley, B., Gee, A.P., Rooney, C.M., Dotti, G., Savoldo, B., Heslop, H.E., and Brenner, M.K.

Subjects

ANTIGEN receptors, HODGKIN'S disease, T cells, CELLULAR therapy, CD30 antigen

Published

2019

15. CD30‐CHIMERIC ANTIGEN RECEPTOR (CAR) T CELLS FOR THERAPY OF HODGKIN LYMPHOMA (HL).

Author

Ramos, C.A., Torrano, V., Bilgi, M., Gerken, C., Dakhova, O., Mei, Z., Wu, M., Grilley, B., Gee, A.P., Rooney, C.M., Dotti, G., Savoldo, B., Heslop, H.E., and Brenner, M.K.

Subjects

ANTIGEN receptors, HODGKIN'S disease, T cells, CELLULAR therapy, CD30 antigen

Published

2019