Literature DB >> 10706056

Stimulated response of peripheral lymphocytes may distinguish cyclosporine effect in renal transplant recipients receiving a cyclosporine+rapamycin regimen.

R Sindhi1, M F LaVia, E Paulling, J McMichael, G Burckart, S Shaw, L A Sindhi, R Livingston, S Sehgal, J Jaffe.   

Abstract

BACKGROUND: Clinically, cyclosporine (CSA, Neoral) is titrated to concentrations, and not to pharmacological effect.
METHODS: Intracellular interleukin- (IL) 2 was measured in phorbol myristic acid-ionomycin-stimulated peripheral lymphocytes by flow cytometry, after isolation from 14 renal transplant recipients receiving CSA+prednisone, and double-blind rapamycin (rapamycin:placebo=4:1).
RESULTS: The proportion (%) of CD4+IL-2+ lymphocytes corresponding to CSA levels (mean+/-SD ng/ml) measured preoperatively (TO=O), and on postoperative day 8, before (356+/-63), and 2 hr after the morning dose (Cmax=1567+/-669), decreased from 39+/-16 to 15+/-8 and 3+/-1.6, respectively. Reciprocally, unresponsive lymphocytes (%CD4+IL-2-) increased with increasing CSA levels and predicted an EC50 of 249 ng/ml (CSA concentration at which CD4+IL-2- cells increased by 50% over baseline) in an Emax pharmacodynamic model.
CONCLUSIONS: Clinically, the pharmacological effect of CSA is quantifiable, and lies in the upper end of the predicted range. In our Neoral-treated sample population, Cmax was associated with the least variable "cyclosporine effect." Such information could potentially individualize immunosuppression, and lead to rational dosing strategies.

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Year:  2000        PMID: 10706056     DOI: 10.1097/00007890-200002150-00022

Source DB:  PubMed          Journal:  Transplantation        ISSN: 0041-1337            Impact factor:   4.939


  8 in total

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Authors:  Tatsuo Furukawa; Tori Kurasaki-Ida; Masayoshi Masuko; Nobuhiro Tsukada; Kiyoshi Okazuka; Naoko Sato; Toshio Yano; Takashi Abe; Akihito Momoi; Yasuhiko Shibasaki; Masutaka Higashimura; Kaori Karimata; Masato Moriyama; Takashi Kuroha; Jun Takizawa; Ken Toba; Miwako Narita; Ichiro Fuse; Masuhiro Takahashi; Yoshifusa Aizawa
Journal:  Int J Hematol       Date:  2010-06-09       Impact factor: 2.490

Review 2.  mTOR activation is a biomarker and a central pathway to autoimmune disorders, cancer, obesity, and aging.

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Review 3.  Impact of absorption profiling on efficacy and safety of cyclosporin therapy in transplant recipients.

Authors:  P Belitsky; S Dunn; A Johnston; G Levy
Journal:  Clin Pharmacokinet       Date:  2000-08       Impact factor: 6.447

4.  Two-hour post-dose cyclosporin A levels in adolescent renal transplant recipients in the late post-transplant period.

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Journal:  Pediatr Nephrol       Date:  2004-03-31       Impact factor: 3.714

5.  Single-dose daily infusion of cyclosporine for prevention of Graft-versus-host disease after allogeneic bone marrow transplantation from HLA allele-matched, unrelated donors.

Authors:  Yuichiro Nawa; Masamichi Hara; Kazushi Tanimoto; Koichi Nakase; Teruhiko Kozuka; Yoshinobu Maeda
Journal:  Int J Hematol       Date:  2006-02       Impact factor: 2.490

6.  Target of rapamycin inhibitors (TOR-I; sirolimus and everolimus) for primary immunosuppression in kidney transplant recipients.

Authors:  Deirdre Hahn; Elisabeth M Hodson; Lorraine A Hamiwka; Vincent Ws Lee; Jeremy R Chapman; Jonathan C Craig; Angela C Webster
Journal:  Cochrane Database Syst Rev       Date:  2019-12-16

7.  Alloreactive CD154-expressing T-cell subsets with differential sensitivity to the immunosuppressant, belatacept: potential targets of novel belatacept-based regimens.

Authors:  Chethan Ashokkumar; Bishu Ganguly; Robert Townsend; Jaimie White; Samantha Levy; Michael Moritz; George Mazariegos; Qing Sun; Rakesh Sindhi
Journal:  Sci Rep       Date:  2015-10-16       Impact factor: 4.379

8.  A review on therapeutic drug monitoring of immunosuppressant drugs.

Authors:  Niloufar Mohammadpour; Sepideh Elyasi; Naser Vahdati; Amir Hooshang Mohammadpour; Jamal Shamsara
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  8 in total

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