2019
DOI: 10.1186/s13046-019-1383-9
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A novel oral micellar fenretinide formulation with enhanced bioavailability and antitumour activity against multiple tumours from cancer stem cells

Abstract: Background An increasing number of anticancer agents has been proposed in recent years with the attempt to overcome treatment-resistant cancer cells and particularly cancer stem cells (CSC), the major culprits for tumour resistance and recurrence. However, a huge obstacle to treatment success is the ineffective delivery of drugs within the tumour environment due to limited solubility, short circulation time or inconsistent stability of compounds that, together with concomitant dose-limiting system… Show more

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Cited by 34 publications
(43 citation statements)
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“…A comparison can be made with a nanoformulation of fenretinide recently developed for oral use. 38 In this case, the fenretinide concentrations in tumor xenografts obtained 3 h after administration of 100 mg/kg fenretinide were 3.44 ug/mL (8.78 μM), 1.71 ug/mL (4.36 μM) and 4.98 ug/mL (12.71 μM) in lung cancer, melanoma and colon cancer xenografts, respectively.…”
Section: Discussionmentioning
confidence: 66%
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“…A comparison can be made with a nanoformulation of fenretinide recently developed for oral use. 38 In this case, the fenretinide concentrations in tumor xenografts obtained 3 h after administration of 100 mg/kg fenretinide were 3.44 ug/mL (8.78 μM), 1.71 ug/mL (4.36 μM) and 4.98 ug/mL (12.71 μM) in lung cancer, melanoma and colon cancer xenografts, respectively.…”
Section: Discussionmentioning
confidence: 66%
“…This may also increase drug concentration in tumors as a result of the increased drug-plasma concentration that affords biodistribution of increased drug amounts in the different body compartments, including the tumor site. 38 However, repeated administration of oral nanoformulations is required to achieve high drug levels in tumors that would be comparable to those achieved by a single administration of a lower drug dose using intravenously injected nanoformulations. Therefore, the high fenretinide concentrations obtained in NB tumors by FLnMs and FnMs accounted for the decrease in tumor growth observed with both nanoformulations compared to controls.…”
Section: Discussionmentioning
confidence: 99%
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“…One reason they have not been investigated further in GBM is that their structures make them unlikely to cross the BBB. Lastly, fenretinide (4-HPR), a synthetic retinoid with an early FDA approval for T-cell lymphoma, has been investigated for its ability to increase ceramide production by p53-independent mechanisms in cancer cells [ 173 , 174 , 175 , 176 ]. While 4-HPR has shown promise in vitro, its poor solubility and bioavailability have limited its use clinically, with both of the glioma clinical trials showing no improvement in progression-free survival at the doses administered ( Table 2 ) [ 175 , 177 ].…”
Section: Altering Sphingolipid Metabolism For Therapeutic Intervenmentioning
confidence: 99%
“…Fenretinide is active in NB [7][8][9][10] and many other cancer types [11][12][13][14][15][16] by multiple mechanisms, [17][18][19][20][21][22] and it has shown efficacy against cancer stem cells. [23][24][25][26][27][28] Lenalidomide is another alternative antitumor agent currently used in the post-consolidation maintenance therapy of multiple myeloma and other hematological malignances. We selected lenalidomide to combine with fenretinide for its antiangiogenic properties and its acceptable toxicity profile.…”
Section: Introductionmentioning
confidence: 99%