Role of the human CD38 molecule in B cell activation and proliferation

Funaro, Ada; Morra, Massimo; Calosso, Liliana; Zini, M G; Ausiello, Clara Maria; Malavasi, Fabio

doi:10.1111/j.1399-0039.1997.tb02703.x

Cited by 117 publications

(118 citation statements)

References 42 publications

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“…Although CD38 is known for its pro-survival signaling (40,41), higher levels of CD38 could also make it more targetable by therapeutic antibodies, such as daratumumab. Indeed, certain agents are already being investigated for their ability to modulate CD38 expression for this purpose.…”

Section: Discussionmentioning

confidence: 99%

Interferon-γ Promotes Antibody-mediated Fratricide of Acute Myeloid Leukemia Cells

Fatehchand¹,

McMichael²,

Reader³

et al. 2016

Journal of Biological Chemistry

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Edited by Peter CresswellAcute myeloid leukemia (AML) is characterized by the proliferation of immature myeloid lineage blasts. Due to its heterogeneity and to the high rate of acquired drug resistance and relapse, new treatment strategies are needed. Here, we demonstrate that IFN␥ promotes AML blasts to act as effector cells within the context of antibody therapy. Treatment with IFN␥ drove AML blasts toward a more differentiated state, wherein they showed increased expression of the M1-related markers HLA-DR and CD86, as well as of Fc␥RI, which mediates effector responses to therapeutic antibodies. Importantly, IFN␥ was able to up-regulate CD38, the target of the therapeutic antibody daratumumab. Because the antigen (CD38) and effector receptor (Fc␥RI) were both simultaneously up-regulated on the AML blasts, we tested whether IFN␥ treatment of the AML cell lines THP-1 and MV4-11 could stimulate them to target one another after the addition of daratumumab. Results showed that IFN␥ significantly increased daratumumab-mediated cytotoxicity, as measured both by 51 Cr release and lactate dehydrogenase release assays. We also found that the combination of IFN␥ and activation of Fc␥R led to the release of granzyme B by AML cells. Finally, using a murine NSG model of subcutaneous AML, we found that treatment with IFN␥ plus daratumumab significantly attenuated tumor growth. Taken together, these studies show a novel mechanism of daratumumab-mediated killing and a possible new therapeutic strategy for AML.

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Section: Discussionmentioning

confidence: 99%

Interferon-γ Promotes Antibody-mediated Fratricide of Acute Myeloid Leukemia Cells

Fatehchand¹,

McMichael²,

Reader³

et al. 2016

Journal of Biological Chemistry

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“…Splenic B cells proliferate in response to IB4 mAb [39]. Addition of anti-CD38 mAbs (either IB4 or T16) to normal bone marrow B cells (Ͼ90% CD38 ϩ ) co-cultured on stromal layers (mostly CD38 Ϫ but CD157 ϩ ) drastically reduces the number of cells recovered after a 7-day culture period [9].…”

Section: B Lymphocytesmentioning

confidence: 99%

“…Biochemical attempts to answer this question by co-precipitation and crosslinking experiments have failed so far [20] but co-capping and co-modulation experiments have been successful. In T cells, CD38 co-localizes with the TCR/CD3 and down-modulation of CD38 also leads to the disappearance of the TCR/CD3 [33,35]. In B lymphocytes, CD38 has this same kind of liaison with CD19 and the B cell receptor (BCR) complex [38,43], and with CD16 (low affinity Fc␥RIII receptor) in NK cells [20].…”

Section: Myeloid Cellsmentioning

confidence: 99%

“…Incubation of peripheral blood T cells or the T cell line Jurkat with IB4 mAb triggers signaling pathways that lead to (1) activation and proliferation [33], (2) transcription of cytokine genes [34], (3) increased intracellular calcium levels, (4) down-modulation of the TCR/CD3 complex, (5) up-regulation of CD5, CD28, CD69, and CD95, and (6) cell death by apoptosis [35].…”

Section: T Lymphocytesmentioning

confidence: 99%

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The metamorphosis of a molecule: from soluble enzyme to the leukocyte receptor CD38

Ferrero

Malavasi

1999

Journal of Leukocyte Biology

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Human CD38 is a 45-kDa type II membrane glycoprotein with an intricate pattern of expression in leukocytes, although evidence is accumulating of its quite widespread expression in cells of nonvascular origin. CD38 is a member of a nascent eukaryotic gene family encoding cytosolic and membrane-bound enzymes whose substrate is NAD, a coenzyme ubiquitously distributed in nature. Functionally, CD38 is an eclectic molecule with the ability not only to catalyze but also to signal, to mobilize calcium, and to adhere to itself, to hyaluronan, and to other ligands. Interaction with CD38 on various leukocyte subpopulations has profound though diverse consequences on their life-span, but these effects seem to be independent of the enzymatic activity of the molecule. CD38 challenges our expectations of a surface molecule and we must sift through its many guises to unmask its true nature. J. Leukoc. Biol. 65: 151-161; 1999.

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“…Otro de los marcadores que se expresa en los progenitores hematopoyéticos comprometidos es la molécula CD38, una glicoproteína expresada por muchos tipos celulares y que desempeña un papel importante en los procesos de activación y proliferación en los linfocitos maduros, además de estar involucrada en los procesos de interacción entre las células (6,7).…”

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Determinación fenotípica de subpoblaciones de células madre derivadas de sangre de cordón umbilical.

Rodríguez¹,

Cuéllar²,

Cuspoca³

et al. 2006

biomedica

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Introducción. La sangre de cordón umbilical humana es una alternativa para la obtención de células madre hematopoyéticas; sin embargo, no es clara la expresión conjunta de los antígenos CD34, CD38 y HLA-DR, ni de antígenos embrionarios asociados con este tipo de muestra. Objetivos. Determinar la expresión en membrana de los antígenos CD34, CD38 y HLA-DR, así como de los antígenos embrionarios SSEA-4 (Specific Stage Embryonic Antigen-4) y CD13. Materiales y métodos. El estudio se realizó en muestras de sangre de cordón umbilical obtenidas de ochenta mujeres en estado de gravidez normal a término que asistieron al servicio de ginecobstetricia del Hospital Universitario San Ignacio. Los antígenos se determinaron mediante citometría de flujo. Resultados. El rango de células CD34+ presentes en sangre de cordón umbilical humana fue mayor al 0,2% (p=0,0010): a partir de esta población el rango de CD34+/ CD38-/ HLA-DR-fue de 0,0153% a 0,0234%, de CD34+/CD38+/HLA-DR-fue de 0,0191% a 0,296%, de CD34+/ CD38-/HLA-DR+ fue de 0,0427% a 0,0676%, y de CD34+/CD38+/HLA-DR+ fue de 0,2427% a 0,5117%. La expresión de los antígenos embrionarios SSEA-4 y CD13 se determinó con el mismo método y se encontraron ocho muestras positivas para la expresión de estos antígenos. Conclusiones. El fenotipo que se expresa con mayor frecuencia en sangre de cordón umbilical corresponde a CD34+ CD38+ HLA DR+; además, el hallazgo de antígenos embrionarios podría indicar que en sangre de cordón umbilical humana existen poblaciones celulares con fenotipos similares a los progenitores celulares adultos multipotentes (Multipotent Adult Progenitor Cells) descritos en médula ósea.Palabras clave: células madre hematopoyéticas, citometría de flujo, cordón umbilical, trasplante de células madre. Phenotypical determinants of stem cell subpopulations derived from human umbilical cord bloodIntroduction. Human umbilical cord blood (HUCB) is a common source of hematopoietic progenitor cells; however, coexpression of CD34, CD38 and HLA DR antigens and of embryonic antigens (SSEA-4 and CD13) have not been described in HUCB. Objective. The current study attempted to identify in HUCB the presence of these antigens. Materials and methods. Cord blood samples were obtained from 80 women with normal pregnancies, who were attending the gynecology-obstetrics service of the San Ignacio Hospital, Bogotá (Colombia). The antigens were identified with a FACS Calibur BDO flow cytometer and a cocktail of monoclonal antibodies.Results. The population of CD34+ cells in HUCB was higher than 0.2% (p=0.001). The levels of additional cell subpopulations were as follows: CD34+/CD38-/HLA-DR-0.015%-0.023%, CD34+/CD38+/HLA-DR-0.019%-0.30%, CD34+/CD38-/HLA-DR+-0.043%-0.068% and CD34+/CD38+/HLA-DR-0.24%-0.51%. Eight samples of the eighty were positive for embryonic markers. The most frequent phenotype in HUCB was CD34+ CD38+ HLA DR+.

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Role of the human CD38 molecule in B cell activation and proliferation

Cited by 117 publications

References 42 publications

Interferon-γ Promotes Antibody-mediated Fratricide of Acute Myeloid Leukemia Cells

Interferon-γ Promotes Antibody-mediated Fratricide of Acute Myeloid Leukemia Cells

The metamorphosis of a molecule: from soluble enzyme to the leukocyte receptor CD38

Determinación fenotípica de subpoblaciones de células madre derivadas de sangre de cordón umbilical.

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