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Featured researches published by Yaffa Beck.


Free Radical Research | 1991

RECOMBINANT HUMAN SUPEROXIDE DISMUTASES: PRODUCTION AND POTENTIAL THERAPEUTICAL USES

Marian Gorecki; Yaffa Beck; Jacob R. Hartman; Meir Fischer; Lola Weiss; Zelig Tochner; Shimon Slavin; Abraham Nimrod

In many pathological situations, tissue damage is caused by cellular generation of superoxide free radicals (O2-). These active species are generated during post-ischemic reperfusion of organs, in hyperoxic tissue, during acute and chronic inflammation and during exposure to ionizing radiation. Exogenous superoxide dismutase (SOD) was shown to significantly prevent such damage. The genes for human cytosolic Cu/ZnSOD and mitochondrial MnSOD were cloned and introduced into an E. coli expression system. The proteins were expressed in high yields and purified to homogeneity, yielding pharmaceutical-grade materials. These enzymes were used in a variety of in vivo animal models for the demonstration of their protective effects against oxidative damage. Comparative pharmacokinetic studies in rats have revealed that the half-life of Cu/ZnSOD was 6-10 min., while that of MnSOD was 5-6 hours, thus indicating that MnSOD may be superior to Cu/ZnSOD for the treatment of chronic diseases. Indeed, MnSOD was found to be effective as an anti-inflammatory agent in the rat carrageenan induced paw edema acute inflammation model. Both enzymes were also effective in ameliorating post-irradiation damage in mice exposed to whole-body or localized chest X-ray radiation.


Journal of Molecular Biology | 1989

Characterization of crystals of genetically engineered human manganese superoxide dismutase

Ulrike Wagner; Moshe M. Werber; Yaffa Beck; Jacob R. Hartman; Felix Frolow; Joel L. Sussman

The genetically engineered human manganese superoxide dismutase crystallizes in space group P2(1)2(1)2 with a = 75.51 A, b = 79.00 A, c = 67.95 A. At room temperature the crystals are not stable against radiation, so we cooled them to 90 K and collected a data set to 3 A resolution at this temperature.


Nucleic Acids Research | 1987

Human Mn superoxide dismutase cDNA sequence

Yaffa Beck; Rachel Oren; Boaz Amit; Avigdor Levanon; Marian Gorecki; Jacob R. Hartman


Archive | 1986

Method of producing high molecular weight sodium hyallronate by fermentation of streptococcus

Abraham Nimrod; Benjamin Greenman; Dov Kanner; Moshe Landsberg; Yaffa Beck


Nature Biotechnology | 1988

Efficient production of active human manganese superoxide dismutase in Escherichia coli

Yaffa Beck; Daniel Bartfeld; Ziva Yavin; Avigdor Levanon; Marian Gorecki; Jacob R. Hartman


Archive | 1988

Human manganese superoxide dismutase and methods of treatment

Jacob R. Hartman; Yaffa Beck; Abraham Nimrod


Archive | 1986

Human manganese superoxide dismintase cDNA, its expression in a host and method of recovery

Yaffa Beck; Jacob R. Hartman


Archive | 1992

Polypeptide analogs of human manganese superoxide dismutase and compositions and complexes thereof

Jacob R. Hartman; Yaffa Beck


Archive | 1995

Methods of use of human manganese superoxide dismutase

Jacob R. Hartman; Yaffa Beck


Archive | 1992

Plasmids for expression and method of producing a human manganese superoxide dimutase analog

Jacob R. Hartman; Yaffa Beck

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Jacob R. Hartman

Weizmann Institute of Science

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Marian Gorecki

Weizmann Institute of Science

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Avigdor Levanon

Weizmann Institute of Science

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Boaz Amit

Weizmann Institute of Science

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Joel L. Sussman

Weizmann Institute of Science

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Lola Weiss

Hebrew University of Jerusalem

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Meir Fischer

Weizmann Institute of Science

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Moshe M. Werber

Weizmann Institute of Science

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Rachel Oren

Weizmann Institute of Science

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