Literature DB >> 15041395

The evolving experience using everolimus in clinical transplantation.

R N Formica1, K M Lorber, A L Friedman, M J Bia, F Lakkis, J D Smith, M I Lorber.   

Abstract

Everolimus is a derivative of sirolimus, a macrocyclic lactone, originally isolated from Streptomyces hygroscopicus. Both everolimus and sirolimus have a similar mechanism of action, exerting potent inhibition of growth factor-induced proliferation of lymphocytes, as well as other hematopoietic and nonhematopoietic cells of mesenchymal origin. Each agent complexes with the FK506 binding protein 12 to inhibit cyclin dependent kinase(s), collectively termed the target of rapamycin (TOR), causing G1-S phase cell cycle arrest. Safety and efficacy have been documented in large-scale, blinded, randomized, international clinical renal and cardiac transplant trials. Everolimus is more hydrophilic, exhibits a shorter elimination half-life (approximately 30 hours), and demonstrates greater relative bioavailability compared to sirolimus. However, similar to the calcineurin inhibitors and sirolimus, everolimus is biotransformed by the cytochrome P450, 3A4 isozyme. Also similar to sirolimus, clinical experiences identified biologically relevant side effects including hyperlipidemia and exacerbation of cyclosporine (CsA)-associated nephrotoxicity. However, also similar to sirolimus, accumulating evidence suggests that the hyperlipidemia can be controlled and the CsA-associated renal effects appear reduced with a low incidence of acute rejection when everolimus is administered in combination with reduced CsA doses. The experience using everolimus in cardiac transplantation has also provided potentially important insights into the consequences of antiproliferative effects on vascular smooth muscle cells and fibroblasts where reduction in intimal expansion was identified by intravascular coronary ultrasound examination among those patients receiving everolimus. Therefore, available results suggest that the introduction of everolimus as the newest TOR inhibitor should enhance therapeutic options for immunosuppression after organ transplantation.

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Year:  2004        PMID: 15041395     DOI: 10.1016/j.transproceed.2004.01.015

Source DB:  PubMed          Journal:  Transplant Proc        ISSN: 0041-1345            Impact factor:   1.066


  10 in total

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Journal:  Pflugers Arch       Date:  2014-09-12       Impact factor: 3.657

3.  Effect of Everolimus on Heterogenous Renal Cancer Cells Populations Including Renal Cancer Stem Cells.

Authors:  Anna Kornakiewicz; Anna M Czarnecka; Mohammed I Khan; Paweł Krasowski; Anna V Kotrys; Cezary Szczylik
Journal:  Stem Cell Rev Rep       Date:  2018-06       Impact factor: 5.739

4.  CYP3A5 genotype does not influence everolimus in vitro metabolism and clinical pharmacokinetics in renal transplant recipients.

Authors:  Nicolas Picard; Koukeb Rouguieg-Malki; Nassim Kamar; Lionel Rostaing; Pierre Marquet
Journal:  Transplantation       Date:  2011-03-27       Impact factor: 4.939

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Authors:  Sebastian I Arriola Apelo; Dudley W Lamming
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7.  Alternative rapamycin treatment regimens mitigate the impact of rapamycin on glucose homeostasis and the immune system.

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Review 8.  Immunosuppression for in vivo research: state-of-the-art protocols and experimental approaches.

Authors:  Rita Diehl; Fabienne Ferrara; Claudia Müller; Antje Y Dreyer; Damian D McLeod; Stephan Fricke; Johannes Boltze
Journal:  Cell Mol Immunol       Date:  2016-10-10       Impact factor: 11.530

9.  Antimycobacterial Effects of Everolimus in a Human Granuloma Model.

Authors:  David Ashley; Joshua Hernandez; Ruoqiong Cao; Kimberly To; Aram Yegiazaryan; Rachel Abrahem; Timothy Nguyen; James Owens; Maria Lambros; Selvakumar Subbian; Vishwanath Venketaraman
Journal:  J Clin Med       Date:  2020-06-29       Impact factor: 4.241

10.  mTOR Inhibitors in Tuberous Sclerosis Complex.

Authors:  Paolo Curatolo; Romina Moavero
Journal:  Curr Neuropharmacol       Date:  2012-12       Impact factor: 7.363

  10 in total

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