Engineering erythrocytes as a novel carrier for the targeted delivery of the anticancer drug paclitaxel

Harisa, Gamaleldin I.; Ibrahim, Mohamed F.; Alanazi, Fars K.; Shazly, Gamal A.

doi:10.1016/j.jsps.2013.06.007

Cited by 36 publications

(22 citation statements)

References 46 publications

(51 reference statements)

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“…Finally, we note that the maximum tolerated dose of docetaxel injected intravenously to mice is ≈250 µg per mouse (10 mg kg −1 ) . Typical dosage for treatment in mice is anywhere between 75 µg per mouse for low dosage up to the experimental maximum tolerated dose for high dosage . In contrast, the sum total TAX content in the transfused mRBCs is only 1 µg per mouse.…”

Section: Resultsmentioning

confidence: 89%

On Command Drug Delivery via Cell‐Conveyed Phototherapeutics

Marvin

Ding

White

et al. 2019

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Herein, the use of red blood cells (RBCs) as carriers of cytoplasmically interned phototherapeutic agents is described. Photolysis promotes drug release from the RBC carrier thereby providing the means to target specific diseased sites. This strategy is realized with a vitamin B12‐taxane conjugate (B12‐TAX), in which the drug is linked to the vitamin via a photolabile CoC bond. The conjugate is introduced into mouse RBCs (mRBCs) via a pore‐forming/pore‐resealing procedure and is cytoplasmically retained due to the membrane impermeability of B12. Photolysis separates the taxane from the B12 cytoplasmic anchor, enabling the drug to exit the RBC carrier. A covalently appended Cy5 antenna sensitizes the conjugate (Cy5‐B12‐TAX) to far red light, thereby circumventing the intense light absorbing properties of hemoglobin (350–600 nm). Microscopy and imaging flow cytometry reveal that Cy5‐B12‐TAX‐loaded mRBCs act as drug carriers. Furthermore, intravital imaging of mice furnish a real time assessment of circulating phototherapeutic‐loaded mRBCs as well as evidence of the targeted photorelease of the taxane upon photolysis. Histopathology confirms that drug release occurs in a well resolved spatiotemporal fashion. Finally, acoustic angiography is employed to assess the consequences of taxane release at the tumor site in Nu/Nu‐tumor‐bearing mice.

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Section: Resultsmentioning

confidence: 89%

On Command Drug Delivery via Cell‐Conveyed Phototherapeutics

Marvin

Ding

White

et al. 2019

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“…However, the activation of apoptosis highlights, as for the nucleated cells, the toxicity of various xenobiotics against these cells. Furthermore, erythrocyte membranes from different species of mammal can be used, not only as a model system but also as a carrier for diverse active substance vehicles . Animal experimentation is more informative than experimentation, but there are major ethical and financial limitations to the approach.…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, erythrocyte membranes from different species of mammal can be used, not only as a model system but also as a carrier for diverse active substance vehicles. 50,51 Animal experimentation is more informative than experimentation, but there are major ethical and financial limitations to the approach. Therefore, in vitro assays represent an alternative method to testing; indeed, in vitro experiments are often used as an initial screen for the toxicity of substances, the evaluation of their cytotoxic mechanisms and the alternative testing methods to replace animal experimentation that the pharmaceutical scientist may use as a guide to assess the safety and utility of a parenteral formulation.…”

Section: Discussionmentioning

confidence: 99%

The use of erythrocyte fragility to assess xenobiotic cytotoxicity

Pagano

Faggio

2015

Cell Biochemistry & Function

166

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The erythrocytes of mammals represent a good model to evaluate the cytotoxicity of molecules, organic and inorganic, natural or synthetic, by cellular damage measure. Indeed, before any investigation on the mechanism of action of different molecules, it is important to perform a cytotoxicity assay. Among the different cytotoxicity assays that assess a possible toxicity in the red blood cells is the rate of haemolysis. This essay is based on the evaluation of the alterations of red cell membranes in the presence of an eventual xenobiotic. Red blood cells are the main cells in circulation, and they are responsible for transporting oxygen; in fact, any alterations of this process could be lethal. The plasma membrane of red blood cells is a multi-component structure such as to confer to these cells their characteristic biconcave shape, high flexibility, elasticity and deformability. However, there are clear signs of cellular suffering if there are any alterations to this structure. One method of toxicity assessment is based on measurement of the efflux of haemoglobin from suspended red blood cells. Haemolysis, and therefore the loss of haemoglobin, is the signal stability of the cell membrane of the erythrocytes. In recent years, the discovery of programmed cell death in mammalian red blood cells presented a diversification of the response to injury by these a-nucleated cells. This review shows that mammals' erythrocytes might serve well as a model cell to study on the cellular and molecular mechanisms of many treatments.

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“…The whole blood was collected from rats by orbital plexus vein and transferred into a tube with heparin sodium for anticoagulation. Then centrifuged at 4 C, 600Âg for 3 min to remove the plasma and leukocytes in the supernatant, and washed three times with 5% isotonic glucose solution at 4 C. A pre-swelling method was used for loading BH into RBCs (Harisa et al, 2014). 100 lL washed packed RBCs were added to 1 mL hypotonic drug solution (5.2 mg/mL NaHCO 3 , 2.5 mg/mL BH after heating), incubated at room temperature for 20 min.…”

Section: Preparation Of Bh-rbcsmentioning

confidence: 99%

Autologous erythrocytes delivery of berberine hydrochloride with long-acting effect for hypolipidemia treatment

Cheng

Liu

et al. 2020

Drug Delivery

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Discovery of novel pharmacological effects of berberine hydrochloride (BH) has made its clinical application valuable. However, further development and applications of BH are hampered by its short halflife and the side effects associated with its intravenous (iv) injection. To improve the hypolipidemia efficacy and reduce side effects, we encapsulated BH into biocompatible red blood cells (RBCs) to explore its sustained-release effect by hypotonic pre-swelling method. From in vitro evaluation, BH loaded RBCs (BH-RBCs) presented similar morphology and osmotic fragility to native RBCs (NRBCs). After the loading process, the BH-RBCs maintained around 69% of Na þ /K þ-ATPase activity of NRBCs and phosphatidylserine externalization value of BH-RBCs was about 26.1 ± 2.9%. The survival test showed that the loaded cells could circulate in plasma for over 9 d. For in vivo evaluation, a series of tests including pharmacokinetics study and hypolipidemic effect were carried out to examine the long-acting effect of BH-RBCs. The results showed that the release of BH in the loaded cells could last for about 5 d and the hypolipidemic effect can still be observed on 5 d after injection. BH-loaded autologous erythrocytes seem to be a promising sustained releasing delivery system with long hypolipidemic effect.

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Engineering erythrocytes as a novel carrier for the targeted delivery of the anticancer drug paclitaxel

Cited by 36 publications

References 46 publications

On Command Drug Delivery via Cell‐Conveyed Phototherapeutics

On Command Drug Delivery via Cell‐Conveyed Phototherapeutics

The use of erythrocyte fragility to assess xenobiotic cytotoxicity

Autologous erythrocytes delivery of berberine hydrochloride with long-acting effect for hypolipidemia treatment

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