Reversal activity of cyclosporin A and its metabolites M1, M17 and M21 in multidrug-resistant cells

Toffoli, Giuseppe; Corona, Giuseppe; Sorio, Roberto; Bertola, Antonella; Boiocchi, Mauro

doi:10.1002/(sici)1097-0215(19970529)71:5<900::aid-ijc32>3.0.co;2-8

Cited by 10 publications

(2 citation statements)

References 31 publications

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“…27,28 However, the effect of CsA in MCF-7 has been barely considered in previously studies as far as we know. We found that CsA could also profoundly increase the DOX level in MCF-7 (1.3-fold), thus indicating the effect of P-gps on chemotherapy.…”

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confidence: 99%

The co-delivery of a low-dose P-glycoprotein inhibitor with doxorubicin sterically stabilized liposomes against breast cancer with low P-glycoprotein expression

Gao¹,

Lin²,

Chen³

et al. 2014

IJN

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Introduction P-glycoprotein (P-gp) inhibitors are usually used to treat tumors that overexpress P-gps. However, most common types of breast cancers, such as Luminal A, are low-P-gp expressing, at least during the initial phases of treatment. Therefore, it would be interesting to know if P-gp inhibitors are still useful in treating low-P-gp-expressing tumors. Methods In the study reported here, the human breast-cancer cell line MCF-7, chosen as a model of Luminal A, was found to be low-P-gp expressing. We designed a novel doxorubicin (DOX) sterically stabilized liposome system co-loaded with the low-dose P-gp inhibitor cyclosporine A (CsA) (DOX/CsA/SSL). Results The co-delivery system showed good size uniformity, high encapsulation efficiency, and a desirable release profile. The cell-uptake and cytotoxicity studies demonstrated that CsA could significantly enhance the intracellular accumulation and toxicity of free DOX and the liposomal DOX in MCF-7 cells. The confocal microscopy and in vivo imaging study confirmed the intracellular and in vivo targeting effect of DOX/CsA/SSL, respectively. Finally, the in vivo study proved that DOX/CsA/SSL could achieve significantly better antitumor effect against MCF-7 tumor than controls, without inducing obvious systemic toxicity. Conclusion This study demonstrated that the co-delivery of a low-dose P-gp inhibitor and liposomal DOX could improve the therapy of low-P-gp-expressing cancer, which is of significance in clinical tumor therapy.

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confidence: 99%

The co-delivery of a low-dose P-glycoprotein inhibitor with doxorubicin sterically stabilized liposomes against breast cancer with low P-glycoprotein expression

Gao¹,

Lin²,

Chen³

et al. 2014

IJN

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“…④ Increasing the conversion of CsA to M17 and other metabolites. The immunosuppressive effect of M17 was same as that of CsA, and its renal toxicity was significant less[16],[25],[26].…”

Section: Discussionmentioning

confidence: 77%

The effects of diltiazem in renal transplantation patients treated with cyclosporine A

Xue

Song

Tian

et al. 2010

Journal of Biomedical Research

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ObjectiveTo investigate the effects of diltiazem and cyclosporine A (CsA) combination therapy on protecting the kidney, promoting graft functioning and improving post-transplanted kidney recovery.MethodsThe blood concentrations of CsA, the condition of the post-transplant kidney, the rate of acute rejection (AR), as well as hepatic and renal toxicity in 636 cases of renal transplant recipients were determined after being treated by CsA, with or without diltiazem.ResultsCompared with the control group which received CsA, mycophenolate mofetil (MMF) and prednisolone (Pred) but lacked diltiazem, the group receiving these agents together with diltiazem required reduced dosage of CsA (P < 0.01), while blood concentrations of CsA were significantly increased (P < 0.01); the recovery time of graft function was reduced from (6.2±1.5) d to (3.9±1.4) d (P < 0.01), and the rate of AR was decreased from 13.2% to 7.9% (P < 0.01).ConclusionIn renal transplantation patients treated with CsA and diltiazem, blood concentrations of CsA were increased while the dosage was decreased. This efficient combination therapy reduced patients' economic burden, at the same time retained kidney function, promoted graft function recovery and decreased hepatic and renal toxicity and the rate of AR.

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Diltiazem co treatment with cyclosporine for induction of disease remission in sight-threatening non-infectious intraocular inflammation

Shalaby

2016

Jpn J Ophthalmol

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Reversal activity of cyclosporin A and its metabolites M1, M17 and M21 in multidrug-resistant cells

Cited by 10 publications

References 31 publications

The co-delivery of a low-dose P-glycoprotein inhibitor with doxorubicin sterically stabilized liposomes against breast cancer with low P-glycoprotein expression

The co-delivery of a low-dose P-glycoprotein inhibitor with doxorubicin sterically stabilized liposomes against breast cancer with low P-glycoprotein expression

The effects of diltiazem in renal transplantation patients treated with cyclosporine A

Diltiazem co treatment with cyclosporine for induction of disease remission in sight-threatening non-infectious intraocular inflammation

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