Mechanistically elucidating the in vitro safety and efficacy of a novel doxorubicin derivative

Alrushaid, Samaa; Zhao, Yunqi; Sayre, Casey L.; Maayah, Zaid H.; Forrest, M. Laird; Senadheera, Sanjeewa N.; Chaboyer, Kevin; Anderson, Hope D.; El‐Kadi, Ayman O.S.; Davies, Neal M.

doi:10.1007/s13346-017-0379-2

Cited by 11 publications

(14 citation statements)

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“…DoxQ was synthesized by conjugating Dox to quercetin via a glycine linker, as previously described [ 14 ].…”

Section: Methodsmentioning

confidence: 99%

“…For this reason, Dox is only currently available as a parenteral treatment administered intravenously. We have previously reported the synthesis of a Dox-quercetin derivative designed to overcome P–gp efflux and CYP inhibition [ 14 ] as quercetin is a natural flavonoid that exhibits inhibitory effects on CYP3A4 and P–gp [ 15 ] and an antioxidant that scavenges free radicals. Our in vitro investigation of DoxQ [ 14 ] revealed that both Dox and quercetin are released from the conjugate over time.…”

Section: Introductionmentioning

confidence: 99%

“…We have previously reported the synthesis of a Dox-quercetin derivative designed to overcome P–gp efflux and CYP inhibition [ 14 ] as quercetin is a natural flavonoid that exhibits inhibitory effects on CYP3A4 and P–gp [ 15 ] and an antioxidant that scavenges free radicals. Our in vitro investigation of DoxQ [ 14 ] revealed that both Dox and quercetin are released from the conjugate over time. Furthermore, DoxQ inhibited CYP3A4, a major metabolic enzyme involved in the first pass effect, and demonstrated higher cellular uptake by P–gp-positive (MDCK–MDR) cells compared to free Dox.…”

Section: Introductionmentioning

confidence: 99%

“…The cardioprotective mechanism of DoxQ involved scavenging ROS, suppression of oxidative stress, and cardiac hypertrophy markers, and also inhibitory effects on CYP1B1, all of which contribute to Dox’s induced cardiotoxicity. Taken together, the in vitro results of DoxQ showed promise at mitigating the cardiotoxicity of Dox and may also mitigate its poor oral bioavailability in vivo by inhibiting CYP3A4 and P–gp [ 14 ]. The antioxidant effects of DoxQ may also mitigate the renal toxicity induced by Dox and improve its overall tolerability in vivo.…”

Section: Introductionmentioning

confidence: 99%

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Pharmacokinetic and Toxicodynamic Characterization of a Novel Doxorubicin Derivative

Alrushaid

Sayre

Yáñez³

et al. 2017

Pharmaceutics

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Doxorubicin (Dox) is an effective anti-cancer medication with poor oral bioavailability and systemic toxicities. DoxQ was developed by conjugating Dox to the lymphatically absorbed antioxidant quercetin to improve Dox’s bioavailability and tolerability. The purpose of this study was to characterize the pharmacokinetics and safety of Dox after intravenous (IV) and oral (PO) administration of DoxQ or Dox (10 mg/kg) and investigate the intestinal lymphatic delivery of Dox after PO DoxQ administration in male Sprague–Dawley rats. Drug concentrations in serum, urine, and lymph were quantified by HPLC with fluorescence detection. DoxQ intact IV showed a 5-fold increase in the area under the curve (AUC)—18.6 ± 1.98 compared to 3.97 ± 0.71 μg * h/mL after Dox—and a significant reduction in the volume of distribution (Vss): 0.138 ± 0.015 versus 6.35 ± 1.06 L/kg. The fraction excreted unchanged in urine (fe) of IV DoxQ and Dox was ~5% and ~11%, respectively. Cumulative amounts of Dox in the mesenteric lymph fluid after oral DoxQ were twice as high as Dox in a mesenteric lymph duct cannulation rat model. Oral DoxQ increased AUC of Dox by ~1.5-fold compared to after oral Dox. Concentrations of β-N-Acetylglucosaminidase (NAG) but not cardiac troponin (cTnI) were lower after IV DoxQ than Dox. DoxQ altered the pharmacokinetic disposition of Dox, improved its renal safety and oral bioavailability, and is in part transported through intestinal lymphatics.

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“…DoxQ was synthesized by conjugating Dox to quercetin via a glycine linker, as previously described [ 14 ].…”

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Pharmacokinetic and Toxicodynamic Characterization of a Novel Doxorubicin Derivative

Alrushaid

Sayre

Yáñez³

et al. 2017

Pharmaceutics

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“…In fact, it was demonstrated that this conjugate inhibits CYP3 A4 and induces higher cellular uptake by P‐gp‐positive cells than doxorubicin only, despite the cleavage of the combined structure over time, leading to free quercetin and doxorubicin. There is also evidence to support the antitumoral activity and overall tolerability of doxorubicin‐quercetin complex, as observed in a triple‐negative murine breast cancer cell line, and decreased cardiotoxicity and renal side effects due to the inhibition of oxidative stress and CYP1B1, besides ROS scavenging property …”

Section: Anthracyclinesmentioning

confidence: 83%

Antitumour Anthracyclines: Progress and Perspectives

2020

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Anthracyclines are ranked among the most effective chemotherapeutics against cancer. They are glycoside drugs comprising the amino sugar daunosamine linked to a hydroxy anthraquinone aglycone, and act by DNA intercalation, oxidative stress generation and topoisomerase II poisoning. Regardless of their therapeutic value, multidrug resistance and severe cardiotoxicity are important limitations of anthracycline treatment that have prompted the discovery of novel analogues. This review covers the most clinically relevant anthracyclines and their development over decades, since the first discovered natural prototypes to recent semisynthetic and synthetic derivatives. These include registered drugs, drug candidates undergoing clinical trials, and compounds under pre‐clinical investigation. The impact of the structural modifications on antitumour activity, toxicity and resistance profile is addressed.

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