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Carboplatin- and Etoposide-Loaded Lactoferrin Protein Nanoparticles for Targeting Cancer Stem Cells in Retinoblastoma In Vitro. / Narayana, Revu V L; Jana, Pritikana; Tomar, Neha et al.
In: Investigative Ophthalmology & Visual Science, Vol. 62, No. 14, 16.11.2021, p. 13.

Research output: Contribution to journalArticlepeer-review

HarvardHarvard

Narayana, RVL, Jana, P, Tomar, N, Prabhu, V, Nair, RM, Manukonda, R, Kaliki, S, Coupland, SE, Alexander, J, Kalirai, H, Kondapi, AK & Vemuganti, GK 2021, 'Carboplatin- and Etoposide-Loaded Lactoferrin Protein Nanoparticles for Targeting Cancer Stem Cells in Retinoblastoma In Vitro', Investigative Ophthalmology & Visual Science, vol. 62, no. 14, pp. 13. https://doi.org/10.1167/iovs.62.14.13

APA

Narayana, R. V. L., Jana, P., Tomar, N., Prabhu, V., Nair, R. M., Manukonda, R., Kaliki, S., Coupland, S. E., Alexander, J., Kalirai, H., Kondapi, A. K., & Vemuganti, G. K. (2021). Carboplatin- and Etoposide-Loaded Lactoferrin Protein Nanoparticles for Targeting Cancer Stem Cells in Retinoblastoma In Vitro. Investigative Ophthalmology & Visual Science, 62(14), 13. https://doi.org/10.1167/iovs.62.14.13

CBE

Narayana RVL, Jana P, Tomar N, Prabhu V, Nair RM, Manukonda R, Kaliki S, Coupland SE, Alexander J, Kalirai H, et al. 2021. Carboplatin- and Etoposide-Loaded Lactoferrin Protein Nanoparticles for Targeting Cancer Stem Cells in Retinoblastoma In Vitro. Investigative Ophthalmology & Visual Science. 62(14):13. https://doi.org/10.1167/iovs.62.14.13

MLA

VancouverVancouver

Narayana RVL, Jana P, Tomar N, Prabhu V, Nair RM, Manukonda R et al. Carboplatin- and Etoposide-Loaded Lactoferrin Protein Nanoparticles for Targeting Cancer Stem Cells in Retinoblastoma In Vitro. Investigative Ophthalmology & Visual Science. 2021 Nov 16;62(14):13. doi: 10.1167/iovs.62.14.13

Author

Narayana, Revu V L ; Jana, Pritikana ; Tomar, Neha et al. / Carboplatin- and Etoposide-Loaded Lactoferrin Protein Nanoparticles for Targeting Cancer Stem Cells in Retinoblastoma In Vitro. In: Investigative Ophthalmology & Visual Science. 2021 ; Vol. 62, No. 14. pp. 13.

RIS

TY - JOUR

T1 - Carboplatin- and Etoposide-Loaded Lactoferrin Protein Nanoparticles for Targeting Cancer Stem Cells in Retinoblastoma In Vitro

AU - Narayana, Revu V L

AU - Jana, Pritikana

AU - Tomar, Neha

AU - Prabhu, Varsha

AU - Nair, Rohini M

AU - Manukonda, Radhika

AU - Kaliki, Swathi

AU - Coupland, Sarah E

AU - Alexander, Jodi

AU - Kalirai, Helen

AU - Kondapi, Anand K

AU - Vemuganti, Geeta K

PY - 2021/11/16

Y1 - 2021/11/16

N2 - Purpose: Cancer stem cells (CSCs) are known to contribute to tumor relapses by virtue of their chemoresistance. With the knowledge that nanoformulations can overcome drug resistance, we evaluated the efficacy and cytotoxicity of clinical-grade carboplatin (CPT)- and etoposide (ETP)-loaded lactoferrin nanoparticles (Lf-Nps) on total, CD133-enriched (non-CSC), and CD133-depleted (CSC) populations of retinoblastoma (Rb) Y79 cells.Methods: Physicochemical properties of drug-loaded Lf-Nps were measured with transmission electron microscopy and attenuated total reflectance-Fourier transform infrared. The encapsulation efficiency, uptake, and release of drug-loaded Lf-Nps were measured using high-performance liquid chromatography and a UV-visible spectrophotometer. Cytotoxicity of the standard and drug-loaded Lf-Nps was evaluated by the MTT assay.Results: The mean (SD) size and encapsulation efficiency of Lf-CPT and Lf-ETP were 61.2 (3.94) nm, 60% and 45.15 (5.85) nm, 38%, respectively, and the drug release efficiency was highest at pH 6. The increased drug uptake and lower release of drug-loaded Lf-Nps were observed in CSC and non-CSC populations compared to their standard forms. The relative increase of drug uptake and sustained intracellular retention of the drug-loaded Lf-Nps compared to standard drugs showed an enhanced cytotoxicity up to 50%, especially in Rb Y79 CSCs (IC50: CPT, 230.3; Lf-CPT, 118.2; ETP, 198.1; and Lf-ETP, 129) compared to non-CSCs.Conclusions: Our study documents an increase in drug uptake, retention, and cytotoxicity of Lf-CPT and Lf-ETP on Y79 CSCs and non-CSCs as compared to their standard drugs in vitro. The reversal of chemoresistance in the CSC population by nanoformulation appears promising with the potential to pave the way for improved targeted therapy and better clinical outcomes.

AB - Purpose: Cancer stem cells (CSCs) are known to contribute to tumor relapses by virtue of their chemoresistance. With the knowledge that nanoformulations can overcome drug resistance, we evaluated the efficacy and cytotoxicity of clinical-grade carboplatin (CPT)- and etoposide (ETP)-loaded lactoferrin nanoparticles (Lf-Nps) on total, CD133-enriched (non-CSC), and CD133-depleted (CSC) populations of retinoblastoma (Rb) Y79 cells.Methods: Physicochemical properties of drug-loaded Lf-Nps were measured with transmission electron microscopy and attenuated total reflectance-Fourier transform infrared. The encapsulation efficiency, uptake, and release of drug-loaded Lf-Nps were measured using high-performance liquid chromatography and a UV-visible spectrophotometer. Cytotoxicity of the standard and drug-loaded Lf-Nps was evaluated by the MTT assay.Results: The mean (SD) size and encapsulation efficiency of Lf-CPT and Lf-ETP were 61.2 (3.94) nm, 60% and 45.15 (5.85) nm, 38%, respectively, and the drug release efficiency was highest at pH 6. The increased drug uptake and lower release of drug-loaded Lf-Nps were observed in CSC and non-CSC populations compared to their standard forms. The relative increase of drug uptake and sustained intracellular retention of the drug-loaded Lf-Nps compared to standard drugs showed an enhanced cytotoxicity up to 50%, especially in Rb Y79 CSCs (IC50: CPT, 230.3; Lf-CPT, 118.2; ETP, 198.1; and Lf-ETP, 129) compared to non-CSCs.Conclusions: Our study documents an increase in drug uptake, retention, and cytotoxicity of Lf-CPT and Lf-ETP on Y79 CSCs and non-CSCs as compared to their standard drugs in vitro. The reversal of chemoresistance in the CSC population by nanoformulation appears promising with the potential to pave the way for improved targeted therapy and better clinical outcomes.

U2 - 10.1167/iovs.62.14.13

DO - 10.1167/iovs.62.14.13

M3 - Article

C2 - 34784412

VL - 62

SP - 13

JO - Investigative Ophthalmology & Visual Science

JF - Investigative Ophthalmology & Visual Science

SN - 1552-5783

IS - 14

ER -