Your search keyword '"Di Noto R"' showing total 6 results

1. Characterization and predicted role of the microRNA expression profile in amnion from obese pregnant women.

Author

Nardelli, C, Iaffaldano, L, Ferrigno, M, Labruna, G, Maruotti, G M, Quaglia, F, Capobianco, V, Di Noto, R, Del Vecchio, L, Martinelli, P, Pastore, L, and Sacchetti, L

Abstract

Maternal obesity and nutrient excess in utero increase the risk of future metabolic diseases. The mechanisms underlying this process are poorly understood, but probably include genetic, epigenetic alterations and changes in fetal nutrient supply. We have studied the microRNA (miRNA) expression profile in amnion from obese and control women at delivery to investigate if a specific miRNA signature is associated with obesity. The expression profile of 365 human miRNAs was evaluated with the TaqMan Array in amnion from 10 obese and 5 control (prepregnancy body mass index (BMI) >30 and <25 kg m(-2), respectively) women at delivery. Target genes and miRNA-regulated pathways were predicted by bioinformatics. Anthropometric and biochemical parameters were also measured in mothers and newborns. Seven miRNAs were expressed only in obese women (miR-422b, miR-219, miR-575, miR-523, miR-579, miR-618 and miR-659), whereas 13 miRNAs were expressed at a higher level and 12 miRNAs at a lower level in obese women than in controls. MicroRNAs significantly downregulated the neurotrophin, cancer/ErbB, mammalian target of rapamycin, insulin, adipocytokine, actin cytoskeleton and mitogen-activated protein kinase signaling pathways. In conclusion, we show that the miRNA profile is altered in amnion during obesity and hypothesize that this could affect pathways important for placental growth and function, thereby contributing to an increase in the newborn's risk of future metabolic diseases. [ABSTRACT FROM AUTHOR]

Published

2014

2. Flow cytometry analysis of acute promyelocytic leukemia: the power of ‘surface hematology’.

Author

Di Noto, R., Mirabelli, P., and Del Vecchio, L.

Subjects

*FLOW cytometry, *LEUKEMIA, *CYTOLOGICAL techniques, *PATHOLOGISTS

Abstract

The article reflects on hematogical flow cytometry for acute promyelocytic leukemia analysis. Hematogical flow cytometry has revealed series of attractive features including lightness, quickness, exactitude, visibility, and multiplicity. Single-cell resolution has made flow cytometry different from any other tool in utilizing diagnostic hematopathology. Furthermore, clinical hematologists stress that a dose of skepticism on the extended use of flow cytometry can reduce residual spaces.

Published

2007

3. Characterization of two novel cell lines, DERL-2 (CD56+/CD3+/Tcry5+) and DERL-7 (CD56+/CD3-/TCRgammadelta-), derived from a single patient with CD56+ non-Hodgkin's lymphoma.

Author

Di Noto, R, Pane, F, Camera, A, Luciano, L, Barone, M, Lo Pardo, C, Boccuni, P, Intrieri, M, Izzo, B, Villa, M R, Macrí, M, Rotoli, B, Sacchetti, L, Salvatore, F, and Del Vecchio, L

Abstract

Two novel IL2-dependent cell lines, DERL-2 and DERL-7, were established from a patient with hepatosplenic gammadelta T cell lymphoma. This patient presented, at diagnosis, two discrete populations of CD56+ cells, one TCRgammadelta+, the second lacking T cell-restricted antigens. The cell lines derived displayed features corresponding to the two cellular components of the disease: DERL-2 was CD56+/CD3+/TcRgammadelta+ while DERL-7 was CD56+/CD3-/TcRgammadelta-. Along with CD56, the two cell lines shared the expression of CD7, CD2, CD158b and CD117. Karyotype analysis showed that both cell lines were near-diploid, with iso-7q and loss of one chromosome 10. In addition, DERL-2 showed 5q+ in all metaphases analyzed, while DERL-7 revealed loss of one chromosome 4. Genotypically, both cell lines shared the same STR pattern at nine loci and demonstrated an identical rearranged pattern of the T cell receptor genes beta, gamma and delta, with respect to the original tumor cells. These data indicated that both cell lines and the original neoplastic populations were T cell-derived and arose from a common ancestor. Among a large panel of cytokines tested, only SCF was able to substitute IL2 in supporting cell proliferation. Moreover, SCF and IL2 acted synergistically, dramatically enhancing cell growth. These cell lines may represent a model to further analyze the overlap area between T and NK cell malignancies, and may provide new information about the synergistic action of IL2 and SCF on normal and neoplastic T/NK cells. [ABSTRACT FROM AUTHOR]

Published

2001

4. JURL-MK1 (c-kit(high)/CD30-/CD40-) and JURL-MK2 (c-kit(low)/CD30+/CD40+) cell lines: 'two-sided' model for investigating leukemic megakaryocytopoiesis.

Author

Di Noto, R, Luciano, L, Lo Pardo, C, Ferrara, F, Frigeri, F, Mercuro, O, Lombardi, M L, Pane, F, Vacca, C, Manzo, C, Salvatore, F, Rotoli, B, and Del Vecchio, L

Abstract

Two novel cell lines (JURL-MK1 and JURL-MK2) have been established from the peripheral blood of a patient in the blastic phase of chronic myelogenous leukemia. The cells grow in a single cell suspension with doubling times of 48 h (JURL-MK1) and 72 h (JURL-MK2). Cytogenetic analysis has shown that JURL-MK1 is hypodiploid whereas JURL-MK2 is near triploid and that both cell lines retain t(9;22). Moreover, JURL-MK1 and JURL-MK2 have a bcr/abl-fused gene with the same junction found in the patient's fresh cells, and both cell lines express the b3/a2 type of hybrid bcr/abl mRNA. The morphology and immunophenotype of these cell lines are reminiscent of megakaryoblasts. In both lines, a limited but consistent percentage of cells expresses gpIIbIIIa (CD41a), gpIIIa (CD61) and CD36, with no expression of gplb (CD42b), glycophorin A, hemoglobin and CD34. Both cell lines are clearly positive for CD33, CD43, CD45RO and CD63, while CD13, CD44, CD54, CD30 and CD40 are specific features of JURL-MK2. Among cytokine receptors, CD117/SCF-R is strongly displayed by a large fraction of JURL-MK1 cells but is hardly detectable on about 20% JURL-MK2 cells. Both cell lines are clearly positive for CD25/IL2R alpha, while a marked expression of CD116/GM-CSF-R and CDw123/IL3R alpha is restricted to JURL-MK2. Induction of cell differentiation in vitro has demonstrated that TPA is able to modulate the JURL-MK1 phenotype, causing an increased expression of platelet-associated antigens. The JURL-MK2 phenotype is easily modulated by both TPA and DMSO, which cause an increased expression of CD41a and CD117 accompanied by a decreased expression of CD30. Proliferation studies demonstrated that JURL-MK1 cell growth is enhanced by stem cell factor, while JURL-MK2 proliferation is unaffected by this cytokine. JURL-MK1 and JURL-MK2 are two novel cell lines with divergent biological features, representing a 'two-sided' model for investigating new aspects of megakaryocytopoiesis. [ABSTRACT FROM AUTHOR]

Published

1997

5. CMRL-T, a novel T-cell line showing asynchronous phenotype (CD34+/CD1a−/TCRαβ+) and dual T-cell receptor β chain.

Author

Di Noto, R., Mirabelli, P., Mariotti, E., Sacchetti, L., Pane, F., Rotoli, B., Pardo, C. Lo., Del Vecchio, L., Mecucci, C., and Salvatore, F.

Subjects

*LETTERS to the editor, *T cell receptors

Abstract

A letter to the editor is presented in response to the article "CMRL-T, a novel T-cell line showing asynchronous phenotype (CD34+/CD1a-/TCRαβ+) and dual T-cell receptor β chain," in the October 26, 2006.

Published

2006

6. Complete remission of refractory anemia following a single high dose of cyclophosphamide.

Author

Ferrara, F., Copia, C., Annunziata, M., di Noto, R., Russo, C., Palmieri, S., Spasiano, A., and del Vecchio, L.

Abstract

We describe a case of stable complete remission in a patient with refractory anemia complicated by severe autoimmune hemolytic anemia, achieved with a single high dose (4 g/m2) of cyclophosphamide (cyclo). Concomitantly, an effective mobilization of CD34-positive cells was induced. Other immunosuppressive approaches including high-dose methylprednisolone, high-dose immunoglobulin, and cyclosporine had been ineffective. This finding suggests that, in selected cases, an immunologic mechanism may mediate cytopenia in myelodysplastic syndromes (MDS). In addition, it demonstrates that successful mobilization of peripheral blood stem cells can be induced with high-dose cyclo in MDS. [ABSTRACT FROM AUTHOR]

Published

1999