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Dive into the research topics where Andrea Marzullo is active.

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Featured researches published by Andrea Marzullo.


British Journal of Cancer | 1999

Bone marrow angiogenesis and mast cell density increase simultaneously with progression of human multiple myeloma

Domenico Ribatti; A Vacca; Beatrice Nico; Fabio Quondamatteo; Roberto Ria; Monica Minischetti; Andrea Marzullo; Rainer Herken; Luisa Roncali; Franco Dammacco

SummaryImmunohistochemical, cytochemical and ultrastructural data showing vivid angiogenesis and numerous mast cells (MCs) in the bone marrow of 24 patients with active multiple myeloma (MM) compared with 34 patients with non-active MM and 22 patients with monoclonal gammopathy of undetermined significance (MGUS) led us to hypothesize that angiogenesis parallels progression of MM, and that MCs participate in its induction via angiogenic factors in their secretory granules.


International Journal of Cancer | 2000

Angiogenesis and mast cell density with tryptase activity increase simultaneously with pathological progression in B-cell non-Hodgkin's lymphomas.

Domenico Ribatti; Angelo Vacca; Andrea Marzullo; Beatrice Nico; Roberto Ria; Luisa Roncali; Franco Dammacco

Node biopsies of 16 benign lymphadenopathies and 72 B‐cell non‐Hodgkins lymphomas (B‐NHLs) were investigated for counts of microvessels, total metachromatic mast cells (MCs) and MCs expressing tryptase, an angiogenesis‐inducing molecule. Counts were higher in B‐NHLs. When grouped according to the Working Formulation (WF) malignancy grades, they were significantly higher in low‐grade B‐NHLs vs. lymphadenopathies and intermediate‐grade vs. low‐grade tumors and there was a further increase in the high‐grade tumors. A high correlation was demonstrated in all groups of tissues between microvessel counts and both total metachromatic and tryptase‐reactive MCs. These results suggest that angiogenesis in B‐NHLs increases with their progression, and that MCs cooperate in its induction via the tryptase contained in their secretory granules. Int. J. Cancer 85:171–175, 2000. ©2000 Wiley‐Liss, Inc.


Glia | 2003

Severe Alterations of Endothelial and Glial Cells in the Blood-Brain Barrier of Dystrophic mdx Mice

Beatrice Nico; Antonio Frigeri; Grazia Paola Nicchia; Patrizia Corsi; Domenico Ribatti; Fabio Quondamatteo; Rainer Herken; Francesco Girolamo; Andrea Marzullo; Maria Svelto; Luisa Roncali

In this study, we investigated the involvement of the blood‐brain barrier (BBB) in the brain of the dystrophin‐deficient mdx mouse, an experimental model of Duchenne muscular dystrophy (DMD). To this purpose, we used two tight junction markers, the Zonula occludens (ZO‐1) and claudin‐1 proteins, and a glial marker, the aquaporin‐4 (AQP4) protein, whose expression is correlated with BBB differentiation and integrity. Results showed that most of the brain microvessels in mdx mice were lined by altered endothelial cells that showed open tight junctions and were surrounded by swollen glial processes. Moreover, 18% of the perivascular glial endfeet contained electron‐dense cellular debris and were enveloped by degenerating microvessels. Western blot showed a 60% reduction in the ZO‐1 protein content in mdx mice and a similar reduction in AQP4 content compared with the control brain. ZO‐1 immunocytochemistry and claudin‐1 immunofluorescence in mdx mice revealed a diffuse staining of microvessels as compared with the control ones, which displayed a banded staining pattern. ZO‐1 immunogold electron microscopy showed unlabeled tight junctions and the presence of gold particles scattered in the endothelial cytoplasm in the mdx mice, whereas ZO‐1 gold particles were exclusively located at the endothelial tight junctions in the controls. Dual immunofluorescence staining of α‐actin and ZO‐1 revealed colocalization of these proteins. As in ZO‐1 staining, the pattern of immunolabeling with anti–α‐actin antibody was diffuse in the mdx vessels and pointed or banded in the controls. α‐actin immunogold electron microscopy showed gold particles in the cytoplasms of endothelial cells and pericytes in the mdx mice, whereas α‐actin gold particles were revealed on the endothelial tight junctions and the cytoskeletal microfilaments of pericytes in the controls. Perivascular glial processes of the mdx mice appeared faintly stained by anti‐AQP4 antibody, while in the controls a strong AQP4 labeling of glial processes was detected at light and electron microscope level. The vascular permeability of the mdx brain microvessels was investigated by means of the horseradish peroxidase (HRP). After HRP injection, extensive perivascular areas of marker escape were observed in mdx mice, whereas HRP was exclusively intravascularly localized in the controls. Inflammatory cells, CD4‐, CD8‐, CD20‐, and CD68‐positive cells, were not revealed in the perivascular stroma of the mdx brain. These findings indicate that dystrophin deficiency in the mdx brain leads to severe injury of the endothelial and glial cells with disturbance in α‐actin cytoskeleton, ZO‐1, claudin‐1, and AQP4 assembly, as well as BBB breakdown. The BBB alterations suggest that changes in vascular permeability are involved in the pathogenesis of the neurological dysfunction associated with DMD. GLIA 42:235–251, 2003.


British Journal of Cancer | 1998

Do mast cells help to induce angiogenesis in B-cell non-Hodgkin's lymphomas?

Domenico Ribatti; Beatrice Nico; A Vacca; Andrea Marzullo; N Calvi; Luisa Roncali; Franco Dammacco

Morphological and morphometric data showing a higher number of mast cells (MCs) in the stroma of B-cell non-Hodgkins lymphomas (B-NHL) than in benign lymphadenopathies are presented in support of the suggestion that angiogenesis during the progression of B-NHL may be partly mediated by angiogenic factors in their secretory granules.


Leukemia | 2002

Correlation of bone marrow angiogenesis and mast cells with tryptase activity in myelodysplastic syndromes.

Domenico Ribatti; G Polimeno; A Vacca; Andrea Marzullo; Enrico Crivellato; Beatrice Nico; Giuseppe Lucarelli; Franco Dammacco

Bone marrow samples from 30 patients with myelodysplastic syndromes (MDS) grouped according to the International Prognostic Scoring System for MDS were investigated for counts of microvessels, total metachromatic mast cells (MC) and MC expressing tryptase, an angiogenesis-inducing molecule. Counts were higher in patients with a poor prognosis. The observation of a high correlation between microvessel counts and both total metachromatic and tryptase-reactive MC in all samples suggests that angiogenesis in MDS increases with their progression and that MC may intervene in the angiogenic response in MDS through tryptase contained in their secretory granules.


International Journal of Experimental Pathology | 2010

Mast cells and angiogenesis in gastric carcinoma

Domenico Ribatti; Diego Guidolin; Andrea Marzullo; Beatrice Nico; Tiziana Annese; Vincenzo Benagiano; Enrico Crivellato

Previous studies have shown that increased vascularity is associated with haematogenous metastasis and poor prognosis in gastric cancer. The role of mast cells in gastric cancer angiogenesis has not been clarified completely. In this study, we correlated microvascular density and tryptase‐ and chymase‐positive mast cells with histopathological type in gastric cancer. Specimens of primary gastric adenocarcinomas obtained from 30 patients who had undergone curative gastrectomy were investigated immunohistochemically by using anti‐CD31 antibody to stain endothelial cells and anti‐tryptase and anti‐chymase antibodies to stain mast cells. The results showed that stage IV gastric carcinoma has a higher degree of vascularization than other stages and that both tryptase‐ and chymase‐positive mast cells increase in parallel with malignancy grade even if the density of chymase‐positive mast cells was significantly lower than the density of tryptase‐positive mast cells and is highly correlated with the extent of angiogenesis. This study has demonstrated that mast cell density correlates with angiogenesis and progression of patients with gastric carcinoma. Understanding the mechanisms of gastric cancer angiogenesis provides a basis for a rational approach to the development of an antiangiogenic therapy in patients with this malignancy.


Histopathology | 2003

Erythropoietin as an angiogenic factor in gastric carcinoma

Domenico Ribatti; Andrea Marzullo; Beatrice Nico; Enrico Crivellato; Roberto Ria; Angelo Vacca

Aims:  Previous studies have shown that increased vascularity is associated with haematogenous metastasis and poor prognosis in gastric cancer. The role of erythropoietin (Epo) in angiogenesis has not been completely clarified, although its involvement has been reported. In this study we correlated microvascular density and Epo receptor (Epo‐R) expression in endothelial and tumour cells with histopathological type in gastric cancer.


Ultrasound in Obstetrics & Gynecology | 2004

Characteristics, associations and outcome of absent pulmonary valve syndrome in the fetus

P. Volpe; D. Paladini; Maurizio Marasini; Antonia Lucia Buonadonna; M. G. Russo; Gilda Caruso; Andrea Marzullo; P. Arciprete; P. Martinelli; Mattia Gentile

To assess in a population of 21 fetuses diagnosed with absent pulmonary valve syndrome (APVS) the accuracy of prenatal diagnosis, the incidence of extracardiac and chromosomal anomalies and the perinatal outcome.


Histopathology | 2007

Erythropoietin/erythropoietin-receptor system is involved in angiogenesis in human hepatocellular carcinoma

Domenico Ribatti; Andrea Marzullo; Antonella Gentile; Longo; Beatrice Nico; Angelo Vacca; Franco Dammacco

Aims:  To correlate microvascular density and erythropoietin (Epo)/Epo‐receptor (EpoR) expression in endothelial and tumour cells with histopathological type in hepatocellular carcinoma (HCC).


European Journal of Clinical Investigation | 2003

Interleukins 1 beta and 6 induce functional alteration of rat colonic motility: an in vitro study

L. Natale; A. L. Piepoli; M. A. De Salvia; G. De Salvatore; C. I. Mitolo; Andrea Marzullo; Piero Portincasa; A. Moschetta; Giuseppe Palasciano; D. Mitolo-Chieppa

Background In rodents, interleukins administration induces intestinal changes similar to those found in inflammatory bowel disease. We investigated the effects of in vivo subchronic treatment with IL‐1 beta and IL‐6 on rat colonic mucosa and circular smooth muscle.

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