Your search keyword '"Parmiani, Giorgio"' showing total 15 results

1. Cannibalism of live lymphocytes by human metastatic but not primary melanoma cells.

Author

Lugini L, Matarrese P, Tinari A, Lozupone F, Federici C, Iessi E, Gentile M, Luciani F, Parmiani G, Rivoltini L, Malorni W, and Fais S

Subjects

Cell Line, Tumor, Cell Survival physiology, Cytoplasmic Vesicles metabolism, Cytoplasmic Vesicles physiology, Humans, Hydrogen-Ion Concentration, Immunohistochemistry, Lymphocytes immunology, Melanoma immunology, Melanoma metabolism, Phagocytosis, T-Lymphocytes immunology, T-Lymphocytes pathology, Lymphocytes pathology, Melanoma pathology, Melanoma secondary

Abstract

The phenomenon of cell cannibalism, which generally refers to the engulfment of cells within other cells, was described in malignant tumors, but its biological significance is still largely unknown. In the present study, we investigated the occurrence, the in vivo relevance, and the underlying mechanisms of cannibalism in human melanoma. As first evidence, we observed that tumor cannibalism was clearly detectable in vivo in metastatic lesions of melanoma and often involved T cells, which could be found in a degraded state within tumor cells. Then, in vitro experiments confirmed that cannibalism of T cells was a property of metastatic melanoma cells but not of primary melanoma cells. In particular, morphologic analyses, including time-lapse cinematography and electron microscopy, revealed a sequence of events, in which metastatic melanoma cells were able to engulf and digest live autologous melanoma-specific CD8(+) T cells. Importantly, this cannibalistic activity significantly increased metastatic melanoma cell survival, particularly under starvation condition, supporting the evidence that tumor cells may use the eating of live lymphocytes as a way to "feed" in condition of low nutrient supply. The mechanism underlying cannibalism involved a complex framework, including lysosomal protease cathepsin B activity, caveolae formation, and ezrin cytoskeleton integrity and function. In conclusion, our study shows that human metastatic melanoma cells may eat live T cells, which are instead programmed to kill them, suggesting a novel mechanism of tumor immune escape. Moreover, our data suggest that cannibalism may represent a sort of "feeding" activity aimed at sustaining survival and progression of malignant tumor cells in an unfavorable microenvironment.

Published

2006

2. Induction of lymphocyte apoptosis by tumor cell secretion of FasL-bearing microvesicles.

Author

Andreola G, Rivoltini L, Castelli C, Huber V, Perego P, Deho P, Squarcina P, Accornero P, Lozupone F, Lugini L, Stringaro A, Molinari A, Arancia G, Gentile M, Parmiani G, and Fais S

Subjects

Blotting, Western, Culture Media, Conditioned, Exocytosis, Fas Ligand Protein, Humans, Immunohistochemistry, Intracellular Membranes metabolism, Jurkat Cells, Lymphocytes immunology, Melanoma immunology, Membrane Glycoproteins immunology, Microscopy, Electron, Secretory Vesicles immunology, Tumor Cells, Cultured, Apoptosis, Lymphocytes cytology, Melanoma metabolism, Melanoma pathology, Melanosomes metabolism, Membrane Glycoproteins metabolism, Secretory Vesicles metabolism

Abstract

The hypothesis that FasL expression by tumor cells may impair the in vivo efficacy of antitumor immune responses, through a mechanism known as 'Fas tumor counterattack,' has been recently questioned, becoming the object of an intense debate based on conflicting results. Here we definitely show that FasL is indeed detectable in the cytoplasm of melanoma cells and its expression is confined to multivesicular bodies that contain melanosomes. In these structures FasL colocalizes with both melanosomal (i.e., gp100) and lysosomal (i.e., CD63) antigens. Isolated melanosomes express FasL, as detected by Western blot and cytofluorimetry, and they can exert Fas-mediated apoptosis in Jurkat cells. We additionally show that melanosome-containing multivesicular bodies degranulate extracellularly and release FasL-bearing microvesicles, that coexpress both gp100 and CD63 and retain their functional activity in triggering Fas-dependent apoptosis of lymphoid cells. Hence our data provide evidence for a novel mechanism potentially operating in Fas tumor counterattack through the secretion of subcellular particles expressing functional FasL. Such vesicles may form a sort of front line hindering lymphocytes and other immunocompetent cells from entering neoplastic lesions and exert their antitumor activity.

Published

2002

3. Adoptive immunotherapy of cancer with immune and activated lymphocytes: Experimental and clinical studies

Author

Parmiani, Giorgio, Sensi, Maria Luisa, Balsari, Andrea, Colombo, Mario P., Gambacorti-Passerini, Carlo, Grazioli, Laura, Rodolfo, Monica, Cascinelli, Natale, and Fossati, Giuseppe

Published

1986

4. Immune landscape and in vivo immunogenicity of NY-ESO-1 tumor antigen in advanced neuroblastoma patients.

Author

Camisaschi, Chiara, Renne, Salvatore Lorenzo, Beretta, Valeria, Rini, Francesca, Spagnuolo, Rosalin Dolores, Tuccitto, Alessandra, Podda, Marta Giorgia, Parmiani, Giorgio, Rivoltini, Licia, Collini, Paola, Castelli, Chiara, and Luksch, Roberto

Subjects

TUMOR antigens, NEUROBLASTOMA, IMMUNOHISTOCHEMISTRY, HLA histocompatibility antigens, LYMPHOCYTES, CLINICAL trials, COMPARATIVE studies, IMMUNOTHERAPY, RESEARCH methodology, MEDICAL cooperation, MEMBRANE proteins, RESEARCH, RESEARCH funding, T cells, CANCER vaccines, EVALUATION research, THERAPEUTICS

Abstract

Background: Indirect evidence suggesting the immunosensitivity/immunogenicity of neuroblastoma is accumulating. The aims of this study were to investigate the immune landscape of neuroblastoma and to evaluate the in vivo immunogenicity of the NY-ESO-1 tumor antigen in advanced neuroblastoma patients.Methods: The immune infiltrating cells of the NY-ESO-1+ tumors from three HLA*A201 patients with metastatic neuroblastoma who relapsed after conventional treatments were evaluated by immunohistochemistry. The patients were vaccinated with the HLA-A*0201-restricted peptide NY-ESO-1157-165(V). The peptide was emulsified in Montanide ISA51 and given subcutaneously in a phase I pilot study. The immunogenicity of NY-ESO-1 antigen was evaluated by monitoring mononuclear cells in patient peripheral blood, pre- and post-vaccine, by short-term in vitro sensitization, HLA-multimer staining and IFN-γ ELISpot analysis.Results: Both CD3 T cells and CD163 myeloid cells were present in pre-vaccine tumors and PD-1 and PD-L1 expression was mainly found in the immune infiltrate. Despite the advanced stage of the disease, the vaccination induced systemic NY-ESO-1 specific CD8 T cells releasing IFN-γ in response to activation with the NY-ESO-1 peptide and an HLA-A2 positive neuroblastoma cell line.Conclusions: Our results indicate that vaccination with a tumor-associated peptide is able to boost NY-ESO-1-specific, functionally active T cells in advanced neuroblastoma patients with lymphocyte infiltration in their pre-vaccine tumors.Trial Registration: EudraCT #2006-002859-33. [ABSTRACT FROM AUTHOR]

Published

2018

5. Ex vivo enrichment of circulating anti-tumor T cells from both cutaneous and ocular melanoma patients: clinical implications for adoptive cell transfer therapy.

Author

Mazzarella, Tonia, Cambiaghi, Valeria, Rizzo, Nathalie, Pilla, Lorenzo, Parolini, Danilo, Orsenigo, Elena, Colucci, Annalisa, Modorati, Giulio, Doglioni, Claudio, Parmiani, Giorgio, and Maccalli, Cristina

Subjects

MELANOMA, CELL transformation, LYMPHOCYTES, IMMUNOTHERAPY, IMMUNE response, CD28 antigen, PATIENTS

Abstract

Tumor-infiltrating lymphocytes (TILs) have been successfully used for adoptive cell transfer (ACT) immunotherapy; however, due to their scarce availability, this therapy is possible for a limited fraction of cutaneous melanoma patients. We assessed whether an effective protocol for ex vivo T-cell expansion from peripheral blood mononuclear cells (PBMCs), suitable for ACT of both cutaneous and ocular melanoma patients, could be identified. PBMCs from both cutaneous and ocular melanoma patients were stimulated in vitro with autologous, irradiated melanoma cells (mixed lymphocyte tumor cell culture; MLTCs) in the presence of IL-2 and IL-15 followed by the rapid expansion protocol (REP). The functional activity of these T lymphocytes was characterized and compared with that of TILs. In addition, the immune infiltration in vivo of ocular melanoma lesions was analyzed. An efficient in vitro MLTC expansion of melanoma reactive T cells was achieved from all PBMC's samples obtained in 7 cutaneous and ocular metastatic melanoma patients. Large numbers of melanoma-specific T cells could be obtained when the REP protocol was applied to these MLTCs. Most MLTCs were enriched in non-terminally differentiated T cells homogeneously expressing co-stimulatory molecules (e.g., NKG2D, CD28, CD134, CD137). A similar pattern of anti-tumor activity, in association with a more variable expression of co-stimulatory molecules, was detected on short-term in vitro cultured TILs isolated from the same patients. In these ocular melanoma patients, we observed an immune infiltrate with suppressive characteristics and a low rate of ex vivo growing TILs (28.5% of our cases). Our MLTC protocol overcomes this limitation, allowing the isolation of T lymphocytes with effector functions even in these patients. Thus, anti-tumor circulating PBMC-derived T cells could be efficiently isolated from melanoma patients by our novel ex vivo enrichment protocol. This protocol appears suitable for ACT studies of cutaneous and ocular melanoma patients. [ABSTRACT FROM AUTHOR]

Published

2012

6. Non-Redundant Role for IL-12 and IL-27 in Modulating Th2 Polarization of Carcinoembryonic Antigen Specific CD4 T Cells from Pancreatic Cancer Patients.

Author

Tassi, Elena, Braga, Marco, Longhi, Renato, Gavazzi, Francesca, Parmiani, Giorgio, Di Carlo, Valerio, and Pia Protti, Maria

Subjects

CANCER patients, T cells, CYTOKINES, IMMUNOREGULATION, CELLULAR immunity, LYMPHOCYTES, TUMOR antigens, CANCER invasiveness, TUMOR markers

Abstract

Background: Pancreatic cancer is a very aggressive disease with dismal prognosis; peculiar is the tumor microenvironment characterized by an extensive fibrotic stroma, which favors rapid tumor progression. We previously reported that pancreatic cancer patients have a selective Th2 skew in the anti-carcinoembryonic antigen (CEA) CD4+ T cell immunity, which correlates with the presence of a predominant GATA-3+ tumor lymphoid infiltrate. This has negative effects in both effective anti-tumor immunity and further favoring fibrinogenesis. Aim of this study was to evaluate whether the Th2 polarization of CEA-specific CD4+ T cells from pancreatic cancer patients is stable or can be reverted by immunomodulating cytokines. Methodology/Principal Findings: We first evaluated the influence of IL-12 and IL-27, as single agents and in association, on the polarization of CEA-specific Th2 CD4+ T cell clones from a pancreatic cancer patient. We found that only the combination of IL-12 and IL-27 modified the polarization of Th2 effectors by both reduction of IL-5, GM-CSF and IL-13 and induction of IFN-γ production, which lasted after cytokine removal. Second, we evaluated the effect of the combined treatment on polyclonal CEA-specific CD4+ T cells in short-time re-stimulation assays. In agreement with the data obtained with the clones, we found that the combined treatment functionally modulated the Th2 polarization of CEA-specific CD4+ T cells and enhanced pre-existing Th1 type immunity. Conclusions/Significance: Collectively, our results demonstrate that tumor antigen specific Th2 CD4+ T cells in pancreatic cancer are endowed with functional plasticity. Hence, loco-regional cytokines delivery or targeted therapy based on antibodies or molecules directed to the tumor stroma might improve anti-tumor immunity and ameliorate fibrosis, without systemic toxicity. [ABSTRACT FROM AUTHOR]

Published

2009

7. TNK cells (NKG2D+ CD8+ or CD4+ T lymphocytes) in the control of human tumors.

Author

Maccalli, Cristina, Scaramuzza, Samantha, and Parmiani, Giorgio

Subjects

IMMUNE response, T cells, LYMPHOCYTES, CANCER cells, LEUCOCYTES

Abstract

Innate and adaptive immune responses have many interactions that are regulated by the balance of signals initiated by a variety of activatory and inhibitory receptors. Among these, the NKG2D molecule was identified as expressed by T lymphocytes, including most CD8+ cells and a minority of CD4+ cells, designated TNK cells in this paper. Tumor cells may overexpress the stress-inducible NKG2D ligands (NKG2DLs: MICA/B, ULBPs) and the NKG2D signaling has been shown to be involved in lymphocyte-mediated anti-tumor activity. Aberrant expression of NKG2DLs by cancer cells, such as the release of soluble form of NKG2DLs, can lead to the impairment of these immune responses. Here, we discuss the significance of NKG2D in TNK-mediated anti-tumor activity. Our studies demonstrate that NKG2D+ T cells (TNK) are commonly recruited at the tumor site in melanoma patients where they may exert anti-tumor activity by engaging both TCR and NKG2D. Moreover, NKG2D and TCR triggering was also observed by peripheral blood derived T lymphocyte- or T cell clone-mediated tumor recognition, both in melanoma and colorectal cancer (CRC) patients. Notably, heterogeneous expression of NKG2DLs was found in melanoma and CRC cells, with a decrease of these molecules along with tumor progression. Therefore, through the mechanisms that govern NKG2D engagement in anti-tumor activity and the expression of NKG2DLs by tumor cells that still need to be dissected, we showed that NKG2D expressing TNK cells are a relevant T cell subtype for immunosurveillance of tumors and we propose that new immunotherapeutic interventions for cancer patients should be aimed also at enhancing NKG2DLs expression by tumor cells. [ABSTRACT FROM AUTHOR]

Published

2009

8. Update on vaccines for melanoma patients.

Author

Russo, Vincenzo, Maccalli, Cristina, Pilla, Lorenzo, Mercuri, Santo Raffaele, Orsenigo, Elena, Mukenge, Sylvain, Bregni, Marco, and Parmiani, Giorgio

Subjects

MELANOMA, LYMPHOCYTES, VACCINATION, IMMUNIZATION, THERAPEUTICS

Abstract

Vaccination against melanoma has a long history but only recently has this therapeutic approach found a reliable scientific rationale. This review summarizes and updates the knowledge on the role of the main players in the vaccination strategy against metastatic melanoma, that is, the melanoma-associated antigens recognized by T and natural killer T-lymphocytes, the conditions for the immune response to develop and the mechanisms that interfere with it. A commented list of the major vaccination trials whose results have been recently published or are ongoing is also presented. Reasons for failure and potential success are underlines to offer a balanced view of this scientifically exciting but still clinically unrewarding field of investigation. [ABSTRACT FROM AUTHOR]

Published

2008

9. Vaccination therapy in prostate cancer.

Author

Marrari, Andrea, Iero, Manuela, Pilla, Lorenzo, Villa, Sergio, Salvioni, Roberto, Valdagni, Riccardo, Parmiani, Giorgio, and Rivoltini, Licia

Subjects

VACCINATION, PROSTATE cancer, RADIOTHERAPY, PROSTATECTOMY, IMMUNITY, LYMPHOCYTES

Abstract

Radical prostatectomy and radiation therapy provide excellent localized prostate cancer (PC) control. Although the majority of prostate carcinoma is nowadays diagnosed at early stages with favourable risk features, in patients up to 30–40% it recurs within 10 years. Furthermore, the lack of effective therapies, once prostate carcinoma becomes refractory to androgen deprivation, mandates the development of alternative therapeutic options. There is a growing interest in harnessing the potency and specificity of anti-tumour immunity through the generation of fully competent dendritic cells and tumour reactive effector lymphocytes. Several strategies to treat or prevent the development of metastatic PC have been explored in clinical trials and are summarized in this review, considering also the feasibility and safety of these approaches. In some cases clinical responses were achieved showing that vaccine-primed T cells induced anti-tumour activity in vivo. The present findings and perspectives of the immunologic interventions in PC patients will be discussed. [ABSTRACT FROM AUTHOR]

Published

2007

10. Comparative assessment of TCRBV diversity in T lymphocytes present in blood, metastatic lesions, and DTH sites of two melanoma patients vaccinated with an IL-7 gene-modified autologous tumor cell vaccine.

Author

Carsana, Marilisa, Tragni, Gabrina, Nicolini, Gabriella, Bersani, Ilaria, Parmiani, Giorgio, Anichini, Andrea, Sun, Yuan Sheng, Möller, Peter, Schadendorf, Dirk, and Sensi, Maria Luisa

Subjects

TUMORS, LYMPHOCYTES, IMMUNE response

Abstract

A phase I clinical trial using autologous, IL-7 gene-modified tumor cells in patients with disseminated melanoma has been recently completed. Although no major clinical responses were observed, increased antitumor cytotoxicity was measured in postvaccine peripheral blood lymphocytes in a subset of treated patients. To analyze the in situ immune response, the T cell receptor β-chain variable region (BV) repertoire of T cells infiltrating postvaccine lesions was studied in two patients, and compared with that of T cells present in prevaccine ones, in peripheral blood lymphocytes, and, in one patient, in delayed type hypersensitivity (DTH) sites of autologous melanoma inoculum. A relative expansion of T cells expressing few BVs was observed in all postvaccine metastases, and their intratumoral presence was confirmed by immunohistochemistry. Length pattern analysis of the complementarity determining region 3 (CDR3) indicated that the repertoire of T cells expressing some of these BVs was heterogeneous. At difference, CDR3, β-chain joining region usage, and sequence analysis enabled us to demonstrate, within a T-cell subpopulation commonly expanded at DTH sites and at the postvaccine lesion of patient 1, that both DTH sites contained identical dominant T-cell clonotypes. One of them was also expressed at increased relative frequency in the postvaccine lesion compared to prevaccine specimens. These results provide evidence for immunological changes, including in situ clonally expanded T cells, in metastases of patients vaccinated with IL-7 gene-transduced cells. [ABSTRACT FROM AUTHOR]

Published

2002

11. Simultaneous transduction of B7-1 and IL-2 genes into human melanoma cells to be used as vaccine: enhancement of stimulatory activity for autologous and allogeneic lymphocytes.

Author

Mazzocchi, Arabella, Melani, Cecilia, Rivoltini, Licia, Castelli, Chiara, Del Vecchio, Michele, Lombardo, Claudia, Colombo, Mario P., and Parmiani, Giorgio

Subjects

NEUROENDOCRINE tumors, MELANOMA, LEUCOCYTES, LYMPHOCYTES, ANTINEOPLASTIC agents, INTERLEUKIN-2, ANTIVIRAL agents

Abstract

In order to construct an immunogenic cellular vaccine, we transduced three HLA-A*0201 human melanoma lines, selected for expression of classes I and II HLA, adhesion molecules and the T cell-defined melanoma antigens Melan/MART-1, gp100 and tyrosinase, with both interleukin-2 (IL-2) and B7-1 genes by the use of a polycistronic retroviral vector. The lines were selected to share only the HLA-A*0201 allele to avoid generation of strong alloreactivity in case of their multiple in vivo use in HLA-A*0201 + patients. Phenotypic and functional analysis of B7-1-IL2 transduced melanoma lines in comparison with B7-1 transduced and/or parental untransduced counterparts were then carried out. Tumor cells expressing either B7-1 or both genes did not change their original antigenic profile. From a functional point of view, expression of both genes in melanoma lines: (1) improved the response of anti-melanoma cytotoxic T lymphocytes (CTL) over singly transduced or untransduced melanoma cells when subthreshold levels of MHC-peptide complexes were expressed by melanoma cells; (2) conferred a distinct advantage in the ability to stimulate cytotoxicity and interferon-γ release by autologous and/or HLA-A*0201-compatible allogeneic lymphocytes; (3) allowed the generation of a high number of specific CTL by in vitro stimulation of lymphocytes of HLA-A*0201-melanoma patients. Thus, B7-IL2 gene-transduced melanoma lines appear to display a high immunogenicity and could be used as vaccine in melanoma patients. [ABSTRACT FROM AUTHOR]

Published

2001

12. A listing of human tumor antigens recognized by T cells.

Author

Renkvist, Nicolina, Castelli, Chiara, Robbins, Paul F., and Parmiani, Giorgio

Subjects

ANTIGENS, TUMORS, LYMPHOCYTES, LEUCOCYTES, B cells, T cells, SUPPRESSOR cells, INTERLEUKIN-2

Abstract

This article presents a list of human tumor antigens recognized by T cells.

Published

2001

13. Tumor-Infiltrating T Cells — Friend or Foe of Neoplastic Cells?

Author

Parmiani, Giorgio

Subjects

*LYMPHOCYTES, *T cells, *HLA histocompatibility antigens, *COLON cancer

Abstract

The article focuses on the author's views on tumor-infiltrating lymphocytes. He cites pervious studies which found the presence of inflammatory and immune-cell infiltrates in various neoplasms, including colorectal cancer. The author says that new studies in 1990s reported of the presence of HLA-restricted T cells distinct for colorectal cancer in people with tumor-infiltrating lymphocytes and peripheral-blood mononuclear cells from patients with colorectal cancer.

Published

2005

14. Modulation of Microenvironment Acidity Reverses Anergy in Human and Murine Tumor-Infiltrating T Lymphocytes.

Author

Calcinotto, Arianna, Filipazzi, Paola, Grioni, Matteo, Iero, Manuela, De Milito, Angelo, Ricupito, Alessia, Cova, Agata, Canese, Rossella, Jachetti, Elena, Rossetti, Monica, Huber, Veronica, Parmiani, Giorgio, Generoso, Luca, Santinami, Mario, Borghi, Martina, Fais, Stefano, Bellone, Matteo, and Rivoltini, Licia

Subjects

*LYMPHOCYTES, *T cells, *TUMORS, *GLYCOLYSIS, *LACTIC acid

Abstract

Stimulating the effector functions of tumor-infiltrating T lymphocytes (TIL) in primary and metastatic tumors could improve active and adoptive T-cell therapies for cancer. Abnormal glycolysis, high lactic acid production, proton accumulation, and a reversed intra--extracellular pH gradient are thought to help render tumor microenvironments hostile to roving immune cells. However, there is little knowledge about how acidic microenvironments affect T-cell immunity. Here, we report that lowering the environmental pH to values that characterize tumor masses (pH 6-6.5) was sufficient to establish an anergic state in human and mouse tumor-specific CD8+ T lymphocytes. This state was characterized by impairment of cytolytic activity and cytokine secretion, reduced expression of IL-2Rα (CD25) and T-cell receptors (TCR), and diminished activation of STAT5 and extracellular signal--regulated kinase (ERK) after TCR activation. In contrast, buffering pH at physiologic values completely restored all these metrics of T-cell function. Systemic treatment of B16-OVA--bearing mice with proton pump inhibitors (PPI) significantly increased the therapeutic efficacy of both active and adoptive immunotherapy. Our findings show that acidification of the tumor microenvironment acts as mechanism of immune escape. Furthermore, they illustrate the potential of PPIs to safely correct T-cell dysfunction and improve the efficacy of T-cell--based cancer treatments. [ABSTRACT FROM AUTHOR]

Published

2012

15. Targeting TNF-a to Neoangiogenic Vessels Enhances Lymphocyte Infiltration in Tumors and Increases the Therapeutic Potential of Immunotherapy.

Author

Calcinotto, Arianna, Grioni, Matteo, Jachetti, Elena, Curnis, Flavio, Mondino, Anna, Parmiani, Giorgio, Corti, Angelo, and Bellone, Matteo

Subjects

*TUMOR necrosis factors, *LYMPHOCYTES, *IMMUNOTHERAPY, *BLOOD-vessel tumors, *EXTRAVASATION, *CELL adhesion molecules, *CYTOKINES

Abstract

Abnormal tumor vasculature impairs T lymphocyte adhesion to endothelial cells and lymphocyte extravasation into neoplastic tissues, limiting the therapeutic potential of both active and adoptive immunothérapies. We have found that treatment of tumor-bearing mice with NGR-TNF, a Cys-Asn-Gly-Arg-Cys peptide-TNF fusion product capable of altering the endothelial barrier function and improving drug penetration in tumors, associated with the intratumor upregulation of leukocyte-endothelial cell adhesion molecules, the release of proinflammatory cytokines and chemokines, and the infiltration of tumor-specific effector CD8+ T cells. As a result, NGR-TNF enhanced the therapeutic activity of adoptive and active immunotherapy, delaying tumor growth and prolonging survival. Furthermore, we have found that therapeutic effects of these combinations can be further increased by the addition of chemotherapy. Thus, these findings might be relevant for the design of novel immunotherapeutic approaches for cancer patients. [ABSTRACT FROM AUTHOR]

Published

2012