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J Ohara

Researcher at University of Texas Southwestern Medical Center

Publications -  15
Citations -  3222

J Ohara is an academic researcher from University of Texas Southwestern Medical Center. The author has contributed to research in topics: Interleukin 4 & Lymphokine. The author has an hindex of 13, co-authored 15 publications receiving 3194 citations.

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Journal Article

B cell stimulatory factor-1 enhances the IgE response of lipopolysaccharide-activated B cells.

TL;DR: Highly purified BSF-1 from a different source, the T lymphoma cell line EL-4, enhanced IgE production to the same extent as TH supernatants, which suggests that B SF-1 is responsible for this increase in IgEProduction.
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Increased expression of Ia antigens on resting B cells: an additional role for B-cell growth factor.

TL;DR: The results demonstrate that BSF-p1 may play two roles: (i) it acts on resting B cells to increase the levels of Ia antigen expression; and (ii) it sustains the growth of B cells that have been previously activated with mitogens, antigens, or anti-Ig.
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SEROLOGICAL, BIOCHEMICAL, AND FUNCTIONAL IDENTITY OF B CELL-STIMULATORY FACTOR 1 AND B CELL DIFFERENTIATION FACTOR FOR IgG1

TL;DR: It is demonstrated that B cell stimulatory factor (BSF-1) and B cell differentiation factor (BCDF-gamma) are the same lymphokine and that BSF-1 acts on both resting and activated B cells to induce different effects.
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T-cell and mast cell lines respond to B-cell stimulatory factor 1

TL;DR: Evidence is provided that BSF-1 is also responsible for two additional biological activities, the stimulation or maintenance of a state of activation in mouse T-cell lines and the increase in the proliferative rate of certain mast cell lines costimulated with interleukin 3.
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Suppression of in vivo polyclonal IgE responses by monoclonal antibody to the lymphokine B-cell stimulatory factor 1.

TL;DR: Results indicate an important physiologic role for BSF-1 in the generation of IgE antibody responses and suggest means for limiting the production of antibodies responsible for allergic reactions without inhibiting protective antibody responses.