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Dive into the research topics where Sara Blumenstein is active.

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Featured researches published by Sara Blumenstein.


FEBS Letters | 1999

Direct involvement of p53 in the base excision repair pathway of the DNA repair machinery

Hagai Offer; Roland Wolkowicz; Devorah Matas; Sara Blumenstein; Zvi Livneh; Varda Rotter

The p53 tumor suppressor that plays a central role in the cellular response to genotoxic stress was suggested to be associated with the DNA repair machinery which mostly involves nucleotide excision repair (NER). In the present study we show for the first time that p53 is also directly involved in base excision repair (BER). These experiments were performed with p53 temperature‐sensitive (ts) mutants that were previously studied in in vivo experimental models. We report here that p53 ts mutants can also acquire wild‐type activity under in vitro conditions. Using ts mutants of murine and human origin, it was observed that cell extracts overexpressing p53 exhibited an augmented BER activity measured in an in vitro assay. Depletion of p53 from the nuclear extracts abolished this enhanced activity. Together, this suggests that p53 is involved in more than one DNA repair pathway.


Cartilage | 2011

The Chondrogenic Potential of Mesenchymal Cells and Chondrocytes from Osteoarthritic Subjects: A Comparative Analysis.

Gabriel Agar; Sara Blumenstein; Yaron Bar-Ziv; Rami Kardosh; Michal Schrift-Tzadok; Ronit Gal-Levy; Tali Fischler; Revital Goldschmid; Avner Yayon

Objective: The multipotential nature of stem or progenitor cells apparently makes them the ideal choice for any cell therapy, but this as yet remains to be proven. This study (30 subjects) was designed to compare the potential to repair articular cartilage of chondrocytes taken from different regions in osteoarthritic cartilage with that of mesenchymal stem cells prepared from bone marrow of the same subject. Design: Cartilage biopsies, bone marrow, and blood samples were taken from each of 30 individuals with chronic osteoarthritis (aged 62-85 years) undergoing total knee replacement. The chondrogenic potential of chondrocytes isolated from cartilage biopsies taken from different regions of osteoarthritic cartilage was compared with that of mesenchymal cells by quantitative analysis of several chondrocyte specific markers and an ex vivo cartilage differentiation assay. Results: Cartilage-derived articular chondrocytes are superior to bone marrow–derived cells when compared for their ex vivo chondrogenic potential. Interestingly, there was marked and significant difference in the expression of chondrocytic markers between chondrocytes derived from adjacent, visually distinct regions of the diseased cartilage. When cultured in the presence of a fibroblast growth factor 2 variant, all cell samples from both tissues showed a high degree of chondrogenic potential. Conclusions: Although bone marrow–derived mesenchymal cells, when supplemented with the appropriate chondrogenic factors, are a suitable source for autologous cartilage implantation, adult chondroprogenitor cells, particularly those from moderately affected regions of the osteoarthritic joints, demonstrate superior chondrogenic potential.


Cancer Biomarkers | 2007

Novel molecular targets for risk identification: DNA repair enzyme activities

Tamar Paz-Elizur; Dalia Elinger; Sara Blumenstein; Meir Krupsky; Edna Schechtman; Zvi Livneh

DNA is continuously damaged by environmental agents and by intracellular byproducts of metabolism [1,2]. If left unrepaired, this DNA damage will cause mutations due to miscoding during replication, thereby increasing cancer risk [1,3]. Therefore, DNA repair is expected to be a major mechanism that protects organisms against cancer. Indeed, in several hereditary diseases that cause high predisposition to cancer, the mutated genes associated with the disorder encode defective DNA repair proteins [3].


Journal of the National Cancer Institute | 2003

DNA Repair Activity for Oxidative Damage and Risk of Lung Cancer

Tamar Paz-Elizur; Meir Krupsky; Sara Blumenstein; Dalia Elinger; Edna Schechtman; Zvi Livneh


DNA Repair | 2007

Development of an enzymatic DNA repair assay for molecular epidemiology studies: distribution of OGG activity in healthy individuals.

Tamar Paz-Elizur; Dalia Elinger; Yael Leitner-Dagan; Sara Blumenstein; Meir Krupsky; Alain Berrebi; Edna Schechtman; Zvi Livneh


Archive | 2007

N-terminal fgf variants having increased receptor selectivity and uses thereof

Avner Yayon; Eran Rom; Irina Chumakov; Sara Blumenstein


Archive | 2002

Methods and kits for determining a risk to develop cancer, for evaluating an effectiveness and dosage of cancer therapy and for correlating between an activity of a DNA repair enzyme and a cancer

Zvi Livneh; Tamar Paz-Elizur; Sara Blumenstein


Journal of Biological Chemistry | 1996

Beta*, a UV-inducible smaller form of the beta subunit sliding clamp of DNA polymerase III of Escherichia coli. I. Gene expression and regulation.

Tamar Paz-Elizur; Rami Skaliter; Sara Blumenstein; Zvi Livneh


Archive | 2007

FGF-2 variants having N-terminal deletions and increased receptor selectivity and uses thereof

Avner Yayon; Eran Rom; Irina Chumakov; Sara Blumenstein


Cell and Tissue Banking | 2014

Opiates do not violate the viability and proliferative activity of human articular chondrocytes

Ofir Chechik; Ron Arbel; Moshe Salai; Roy Gigi; Mark Beilin; Ron Flaishon; Ronen Sever; Morsi Khashan; Tomer Ben-Tov; Ronit Gal-Levy; Avner Yayon; Sara Blumenstein

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Zvi Livneh

Weizmann Institute of Science

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Avner Yayon

Weizmann Institute of Science

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Tamar Paz-Elizur

Weizmann Institute of Science

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Eran Rom

Weizmann Institute of Science

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Irina Chumakov

Weizmann Institute of Science

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Dalia Elinger

Weizmann Institute of Science

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Edna Schechtman

Ben-Gurion University of the Negev

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Ronit Gal-Levy

Weizmann Institute of Science

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