NYUHSL Faculty Bibliography

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222

Clinical research. 1988:36(3):A620-A620.DOI:

NEUTROPHIL ACTIVATION - EVIDENCE FOR 2 SOURCES OF DIACYLGLYCEROL DISTINGUISHED BY PROTEIN-I OF N - GONORRHOEAE [Meeting Abstract]

Haines, KA; Reibman, J; Vosshall, L; Weissmann, G

ISI:A1988M818002176

ISSN: 0009-9279

CID: 31518

Transactions of the Association of American Physicians. 1988:101:163-72.DOI:

Neutrophil activation: evidence for two sources of diacylglycerol distinguished by protein I of Neisseria gonorrhoeae

Haines KA; Reibman J; Vosshall L; Weissmann G

PMID: 2855897

ISSN: 0066-9458

CID: 11279

Clinical research. 1987:35(3):A537-A537.DOI:

PHOSPHORYLATION OF THE 47KDA TARGET PROTEIN IS NOT SUFFICIENT FOR SUPEROXIDE ANION PRODUCTION IN NEUTROPHILS [Meeting Abstract]

Reibman, J; Korchak, HM; Haines, KA; Vosshall, LB; Weissmann, G

ISI:A1987G986201698

ISSN: 0009-9279

CID: 31195

Clinical research. 1987:35(3):A613-A613.DOI:

COCAINE DERIVATIVES BLUNT NEUTROPHIL RESPONSES [Meeting Abstract]

Callegari, P; Abramson, S; Philips, M; Haines, K; Reibman, J; Weissmann, G

ISI:A1987G986202148

ISSN: 0009-9279

CID: 31199

Federation proceedings (Federation of American Societies for Experimental Biology). 1987:46(3):987-987.DOI:

NEUTROPHIL ACTIVATION - CHEMOATTRACTANTS DIFFER IN THEIR CAPACITY TO ELICIT PROTEIN-PHOSPHORYLATION [Meeting Abstract]

Reibman, J; Haines, KA; Korchak, HM; Weissmann, G

ISI:A1987G323403916

ISSN: 0014-9446

CID: 31268

Advances in prostaglandin thromboxane & leukotriene research. 1987:17B:890-9.DOI:

Leukotriene B4 paradox: neutrophils can, but will not, respond to ligand-receptor interactions by forming leukotriene B4 or its omega-metabolites

Haines KA; Giedd KN; Rich AM; Reibman J; Korchak HM; Weissmann G

PMID: 2823576

ISSN: 0732-8141

CID: 11433

Journal of cell biology. 1986:103(5):A504-A504.DOI:

SUPEROXIDE ANION GENERATION IN LTB4 ACTIVATED NEUTROPHILS - INADEQUACY OF CYTOSOLIC CALCIUM AND DIACYL GLYCEROL AS SIGNALS [Meeting Abstract]

KORCHAK, HM; VOSSHALL, LB; REIBMAN, J; RICH, AM; HAINES, KA

ISI:A1986E958901884

ISSN: 0021-9525

CID: 41326

Clinical research. 1986:34(2):A719-A719.DOI:

DIACYL GLYCEROL INCREMENTS PRECEDE RISES OF CYTOSOLIC CALCIUM IN NEUTROPHIL ACTIVATION - A MODE OF ACTION OF CYTOCHALASIN-B [Meeting Abstract]

KORCHAK, HM; VOSSHALL, LB; REIBMAN, J; VIENNE, K; RICH, AM; WILKENFELD, C; WEISSMANN, G

ISI:A1986C539802644

ISSN: 0009-9279

CID: 41412

American review of respiratory disease. 1986:133(4):A134-A134.DOI:

BETA-ADRENERGIC STIMULATION ALTERS FUNCTION BUT NOT CALCIUM MOVEMENTS IN HUMAN-NEUTROPHILS [Meeting Abstract]

REIBMAN, J; KORCHAK, HM; WILKENFELD, C; RUTHERFORD, L; WEISSMANN, G

ISI:A1986A740800491

ISSN: 0003-0805

CID: 41467

Journal of immunology (1950). 1986:136(3):1027-32.DOI:

Colchicine inhibits ionophore-induced formation of leukotriene B4 by human neutrophils: the role of microtubules

Reibman J; Haines KA; Rich AM; Cristello P; Giedd KN; Weissmann G

Neutrophils which ingest particles (serum-treated zymosan, monosodium urate crystals) or are exposed to calcium ionophore A23187 generate leukotriene B4 (LTB4). Earlier work has shown that cells exposed to colchicine before exposure to monosodium urate crystals produce less LTB4; the formation of 5-HETE is unaffected. To determine whether inhibition by colchicine of LTB4 generation was stimulus-specific and was mediated by microtubule integrity, the effects of colchicine (10 microM, 60 min) on the release of lipoxygenase products from neutrophils exposed to ionophore A23187 (10 microM, 5 min) were examined. In the presence of exogenous arachidonic acid (100 microM, 15 min), colchicine decreased LTB4 to 48% +/- 11.7 of control and 5-HETE to 60.5% +/- 5.7 of control (mean +/- SEM); 15-HETE was also decreased to 61% +/- 10.3 of control. In the absence of exogenous arachidonate, LTB4 was decreased to 22.2% +/- 11.7 of control and 5-HETE to 13% +/- 4.8 of control. Lumicolchicine did not significantly affect formation of 5-HETE or LTB4. However, vinblastine sulfate (20 microM, 60 min), another microtubule-disruptive agent, decreased the formation of both 5-lipoxygenase products. The effects of colchicine and vinblastine were not due to impairment of cell viability because the release of cytoplasmic lactic dehydrogenase was unaffected. Ultrastructural analysis of centriolar microtubules showed that decrements in microtubule numbers of colchicine- and vinblastine-treated cells paralleled decrements in 5-lipoxygenase products. These pharmacologic manipulations suggested that functional microtubules might be required for optimal lipoxygenase activity. Consequently, we prepared neutrophil-derived cytoplasts, devoid of an intact microtubule system. No significant decreases in the 5- or 15-lipoxygenase products were found when cytoplasts were exposed to colchicine in the presence of exogenous arachidonate and A23187. The data show that colchicine inhibits the formation of lipoxygenase products from neutrophils stimulated with A23187, most likely via its effect on microtubules, the integrity of which appears necessary for full expression of 5- and 15-lipoxygenases

PMID: 3001184

ISSN: 0022-1767

CID: 59695