Your search keyword '"El-Hachem, Nehme"' showing total 8 results

1. Gene isoforms as expression-based biomarkers predictive of drug response in vitro.

Author

Safikhani, Zhaleh, Smirnov, Petr, Thu, Kelsie L., Silvester, Jennifer, El-Hachem, Nehme, Quevedo, Rene, Lupien, Mathieu, Mak, Tak W., Cescon, David, and Haibe-Kains, Benjamin

Subjects

PHARMACOGENOMICS, RNA sequencing, TUMOR markers, BREAST cancer, LAPATINIB, ERLOTINIB, PACLITAXEL

Abstract

Next-generation sequencing technologies have recently been used in pharmacogenomic studies to characterize large panels of cancer cell lines at the genomic and transcriptomic levels. Among these technologies, RNA-sequencing enable profiling of alternatively spliced transcripts. Given the high frequency of mRNA splicing in cancers, linking this feature to drug response will open new avenues of research in biomarker discovery. To identify robust transcriptomic biomarkers for drug response across studies, we develop a meta-analytical framework combining the pharmacological data from two large-scale drug screening datasets. We use an independent pan-cancer pharmacogenomic dataset to test the robustness of our candidate biomarkers across multiple cancer types. We further analyze two independent breast cancer data-sets and find that specific isoforms of IGF2BP2, NECTIN4, ITGB6, and KLHDC9 are significantly associated with AZD6244, lapatinib, erlotinib, and paclitaxel, respectively. Our results support isoform expressions as a rich resource for biomarkers predictive of drug response. [ABSTRACT FROM AUTHOR]

Published

2017

2. Consistency in drug response profiling.

Author

Safikhani, Zhaleh, El-Hachem, Nehme, Smirnov, Petr, Freeman, Mark, Goldenberg, Anna, Birkbak, Nicolai J., Beck, Andrew H., Aerts, Hugo J. W. L., Quackenbush, John, and Haibe-Kains, Benjamin

Published

2016

3. Safikhani et al. reply.

Author

Safikhani, Zhaleh, El-Hachem, Nehme, Smirnov, Petr, Freeman, Mark, Goldenberg, Anna, Birkbak, Nicolai J., Beck, Andrew H., Aerts, Hugo J. W. L., Quackenbush, John, and Haibe-Kains, Benjamin

Published

2016

4. Inconsistency in large pharmacogenomic studies.

Author

Haibe-Kains, Benjamin, El-Hachem, Nehme, Birkbak, Nicolai Juul, Jin, Andrew C., Beck, Andrew H., Aerts, Hugo J. W. L., and Quackenbush, John

Subjects

*PHARMACOGENOMICS, *GENOMICS, *ANTINEOPLASTIC agents, *HEALTH outcome assessment, *MEDICAL databases

Abstract

Two large-scale pharmacogenomic studies were published recently in this journal. Genomic data are well correlated between studies; however, the measured drug response data are highly discordant. Although the source of inconsistencies remains uncertain, it has potential implications for using these outcome measures to assess gene-drug associations or select potential anticancer drugs on the basis of their reported results. [ABSTRACT FROM AUTHOR]

Published

2013

5. New analogues of 13-hydroxyocatdecadienoic acid and 12-hydroxyeicosatetraenoic acid block human blood platelet aggregation and cyclooxygenase-1 activity.

Author

Hirz, Taghreed, Khalaf, Ali, El-Hachem, Nehme, Mrad, May F., Abdallah, Hassan, Créminon, Christophe, Grée, René, Abou Merhi, Raghida, Habib, Aïda, Hachem, Ali, and Hamade, Eva

Subjects

THROMBOXANES, ARACHIDONIC acid, CYCLOOXYGENASES, BLOOD platelet aggregation, PHENOLS, HYDROCARBONS

Abstract

Background: Thromboxane A2 is derived from arachidonic acid through the action of cyclooxygenases and thromboxane synthase. It is mainly formed in blood platelets upon activation and plays an important role in aggregation. Aspirin is effective in reducing the incidence of complications following acute coronary syndrome and stroke. The anti-thrombotic effect of aspirin is obtained through the irreversible inhibition of cyclooxygenases. Analogues of 12-hydroxyeicosatetraenoic acid and 13-hydroxyocatdecadienoic acid were shown previously to modulate platelet activation and to block thromboxane receptors. Results and discussion: We synthesized 10 compounds based on the structures of analogues of 12-hydroxyeicosatetraenoic acid and 13-hydroxyocatdecadienoic acid and evaluated their effect on platelet aggregation triggered by arachidonic acid. The structure activity relationship was evaluated. Five compounds showed a significant inhibition of platelet aggregation and highlighted the importance of the lipidic hydrophobic hydrocarbon chain and the phenol group. Their IC50 ranged from 7.5 ± 0.8 to 14.2 ± 5.7 μM (Mean ± S.E.M.). All five compounds decreased platelet aggregation and thromboxane synthesis in response to collagen whereas no modification of platelet aggregation in response to thromboxane receptor agonist, U46619, was observed. Using COS-7 cells overexpressing human cyclooxygenase-1, we showed that these compounds are specific inhibitors of cyclooxygenase-1 with IC50 ranging from 1.3 to 12 μM. Docking observation of human recombinant cyclooxygenase-1 supported a role of the phenol group in the fitting of cyclooxygenase-1, most likely related to hydrogen bonding with the Tyr 355 of cyclooxygenase-1. Conclusions: In conclusion, the compounds we synthesized at first based on the structures of analogues of 12 lipoxygenase metabolites showed a role of the phenol group in the anti-platelet and anti-cyclooxygenase-1 activities. These compounds mediate their effects via blockade of cyclooxygenase-1. [ABSTRACT FROM AUTHOR]

Published

2012

6. Drug response consistency in CCLE and CGP.

Author

Safikhani, Zhaleh, El-Hachem, Nehme, Smirnov, Petr, Freeman, Mark, Goldenberg, Anna, Birkbak, Nicolai J., Beck, Andrew H., Aerts, Hugo J. W. L., Quackenbush, John, and Haibe-Kains, Benjamin

Published

2016

7. gem-Difluorobisarylic derivatives: design, synthesis and anti-inflammatory effect.

Author

Ayoub, Abeer J., Hariss, Layal, El-Hachem, Nehme, El-Achkar, Ghewa A., Ghayad, Sandra E., Dagher, Oula K., Borghol, Nada, Grée, René, Badran, Bassam, Hachem, Ali, Hamade, Eva, and Habib, Aida

Subjects

ANTI-inflammatory agents, ETHERS, KETONES, CYCLOOXYGENASE 2, DINOPROSTONE

Abstract

Introduction: New fluorinated diaryl ethers and bisarylic ketones were designed and evaluated for their anti-inflammatory effects in primary macrophages. Methods: The synthesis of the designed molecules started from easily accessible and versatile gem-difluoro propargylic derivatives. The desired aromatic systems were obtained using Diels–Alder/aromatization sequences and this was followed by Pd-catalyzed coupling reactions and, when required, final functionalization steps. Both direct inhibitory effects on cyclooxygenase-1 or -2 activities, protein expression of cyclooxygenase-2 and nitric oxide synthase-II and the production of prostaglandin E2, the pro-inflammatory nitric oxide and interleukin-6 were evaluated in primary murine bone marrow-derived macrophages in response to lipopolysaccharide. Docking of the designed molecules in cyclooxygenase-1 or -2 was performed. Results: Only fluorinated compounds exerted anti-inflammatory activities by lowering the secretion of interleukin-6, nitric oxide, and prostaglandin E2, and decreasing the protein expression of inducible nitric oxide synthase and cyclooxygenase-2 in mouse primary macrophages exposed to lipopolysaccharide, as well as cyclooxygenase activity for some inhibitors with different efficiencies depending on the R-groups. Docking observation suggested an inhibitory role of cyclooxygenase-1 or -2 for compounds A3, A4 and A5 in addition to their capacity to inhibit nitrite, interleukin-6, and nitric oxide synthase-II and cyclooxygenase-2 expression. Conclusion: The new fluorinated diaryl ethers and bisarylic ketones have anti-inflammatory effects in macrophages. These fluorinated compounds have improved potential anti-inflammatory properties due to the fluorine residues in the bioactive molecules. [ABSTRACT FROM AUTHOR]

Published

2019

8. Author Correction: Gene isoforms as expression-based biomarkers predictive of drug response in vitro.

Author

Smirnov, Petr, Safikhani, Zhaleh, Quevedo, Rene, Lupien, Mathieu, Mak, Tak W., Haibe-Kains, Benjamin, Thu, Kelsie L., Silvester, Jennifer, Cescon, David, and El-Hachem, Nehme

Subjects

GENES, BIOLOGICAL tags

Abstract

A correction is presented to the article “Gene isoforms as expression-based biomarkers predictive of drug response in vitro" which appeared in the 24 October 2017 issue.

Published

2018