N. Galassi scite author profile

N. Galassi

4Publications

84Citation Statements Received

120Citation Statements Given

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117

Affiliations

Academia Nacional de Medicina, University of Buenos Aires, Consejo Nacional de Investigaciones Científicas y Técnicas

Publications

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Common Variable Immunodeficiency and Circulating T_FH

Coraglia

Galassi

Romero

et al. 2016

Journal of Immunology Research

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CD4+ T follicular helper cells (TFH) were assessed in adult patients with common variable immune deficiency (CVID) classified according to the presence of granulomatous disease (GD), autoimmunity (AI), or both GD and AI (Group I) or the absence of AI and GD (Group II). TFH lymphocytes were characterized by expression of CXCR5 and PD-1. TFH were higher (in both absolute number and percentage) in Group I than in Group II CVID patients and normal controls (N). Within CXCR5+CD4+ T cells, the percentage of PD-1 (+) was higher and that of CCR7 (+) was lower in Group I than in Group II and N. The percentages of Treg and TFH reg were similar in both CVID groups and in N. TFH responded to stimulation increasing the expression of the costimulatory molecules CD40L and ICOS as did N. After submitogenic PHA+IL-2 stimulation, intracellular expression of TFH cytokines (IL-10, IL-21) was higher than N in Group I, and IL-4 was higher than N in Group II. These results suggest that TFH are functional in CVID and highlight the association of increased circulating TFH with AI and GD manifestations.

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A flow cytometry evaluation of anti-FVIII antibodies: correlation with ELISA and Bethesda assay

Irigoyen

Primiani

Felippo

et al. 2010

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In this study, we describe a flow cytometry (FC) system for detecting antibodies to factor VIII (FVIII) and compare its results with those of enzyme-linked immunosorbent assay (ELISA) that detects both inhibitory (I-Ab) and non-inhibitory (NI-Ab) antibodies and the Nijmegen modification of the Bethesda method, detecting I-Ab. FC was set up in our laboratory. Recombinant FVIII (rFVIII) was coupled to microspheres (FVIII-m) and reacted with different plasma dilutions. Microspheres without rFVIII were used as control (control-m). Captured anti-FVIII antibodies were detected using anti-human IgG. Plasma samples from the following patients with severe haemophilia A (SHA) patients were evaluated: 17 P (patients without I-Ab, <0.5 BU mL(-1)); 13 PI (patients with I-Ab, 1.1-8200 BU mL(-1)). Of these 13, two PI were referred during immune tolerance induction (ITI), and plasmas from 12 healthy donors (HD) were evaluated. Semiquantitative results were given as an index (the highest mean fluorescence intensity ratio between FVIII-m and control-m multiplied by the inverse of the corresponding plasma dilution). Both plasma and serum were suitable for the test. FC agreed with the Bethesda method (r = 0.8; P = 0.0001). FC and ELISA had 80% of coincidence. Four of 17 patients (23.5%) had NI-Ab by FC, and two of them developed high levels of I-Ab later on. This test provides a useful alternative for measuring FVIII antibodies supplementing Bethesda assay. FC is fast and easy to perform. No more than 200 μL of plasma or serum is required especially making it useful for paediatric patients.

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Diclofenac induces basophil degranulation without increasing CD63 expression in sensitive patients

Malbrán

Yeyati²,

Rey³

et al. 2006

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SummaryDiclofenac (Dc) induces an IgE-independent basophil (Ba) degranulation in susceptible individuals. CD63 Ba expression is utilized as an in vitro test for diagnosis of drug hypersensitivity. We tested the ability of Dc to induce CD63 Ba expression by flow cytometry (BAT) and Ba degranulation using light microscopy (HBDT) in patients sensitive to Dc. We studied 14 patients with diclofenac hypersensitivity, also two patients sensitive to Dermatophagoides pteronyssinus (Dp), and 12 normal controls. HBDT was performed by mononuclear cells toluidine blue staining. BAT determined CD63 expression in antiCD63/anti-IgE/anti-CD45-labelled whole blood. In each case, the percentage of activated Ba post-stimulation with 1 and 10 mg/ml Dc was determined. Positive controls included N-formyl-methionyl-leucyl-phenylalanine (fMLP) peptide-induced activation. IgE-mediated Ba activation was induced with a Dp allergenic extract. With Dc 1 mg/ml, mean HBDT in Dc-susceptible individuals was 33·62 Ϯ 18·35% and 8·49 Ϯ 4·79% in controls (P = 0·0001). Mean BAT was 2·04 Ϯ 1·68% and 1·93 Ϯ 1·40% in controls (P = 0·8). Ba preincubation with Dc did not affect fMLP-induced CD63 expression, neither in Dc-sensitive individuals (P = 0·8) (n = 4) nor in subjects without Dc hypersensitivity (P = 0·25) (n = 4). Ba from the two patients sensitive both to Dc and Dp responded to Dp but not to Dc by BAT: Dc, 1·99 Ϯ 0·78%; Dp: 60·87 Ϯ 9·28%; but showed degranulation by HBDT: Dc, 30·53 Ϯ 1·02%, Dp: 48·78 Ϯ 22·17%. Dc induces Ba degranulation in sensitive patients in a way that does not induce CD63 expression and is different from IgE-mediated and fMLP-mediated degranulation. Our results suggest that CD63 expression is not a reliable diagnostic method for diclofenac allergy.

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Anti-leukocyte antibodies as a consequence of HIV infection in HIV+ individuals

et al. 1992

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N. Galassi

Common Variable Immunodeficiency and Circulating T_FH

A flow cytometry evaluation of anti-FVIII antibodies: correlation with ELISA and Bethesda assay

Diclofenac induces basophil degranulation without increasing CD63 expression in sensitive patients

Anti-leukocyte antibodies as a consequence of HIV infection in HIV+ individuals

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N. Galassi

Common Variable Immunodeficiency and Circulating TFH

A flow cytometry evaluation of anti-FVIII antibodies: correlation with ELISA and Bethesda assay

Diclofenac induces basophil degranulation without increasing CD63 expression in sensitive patients

Anti-leukocyte antibodies as a consequence of HIV infection in HIV+ individuals

Contact Info

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Resources

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Common Variable Immunodeficiency and Circulating T_FH