Delivering Drugs to Cancer Cells and inside the Mitochondria Using a Dual-Ligand Installed Targeted Drug Delivery System

Purvi Kishore; Sourav Barman; Rimpa Dey; Ankita Jana; Malabika Ghosh; Pousali Bag; Tapas Ghatak; Partha Sona Maji; Chitrita Ghosh; Nayana Mukherjee; Ankan Dutta Chowdhury; Souvik Ghatak; Rupam Mukherjee; Arnab Basu; Ali Hossain Khan; Surya K. Ghosh; Sadananda Mandal; Amit Ranjan Maity

doi:10.1021/acsanm.5c04231

Delivering Drugs to Cancer Cells and inside the Mitochondria Using a Dual-Ligand Installed Targeted Drug Delivery System

Purvi Kishore, Sourav Barman, Rimpa Dey, Ankita Jana, Malabika Ghosh, Pousali Bag, Tapas Ghatak, Partha Sona Maji, Chitrita Ghosh, Nayana Mukherjee, Ankan Dutta Chowdhury, Souvik Ghatak, Rupam Mukherjee, Arnab Basu, Ali Hossain Khan, Surya K. Ghosh, Sadananda Mandal, Amit Ranjan Maity

Research output: Contribution to journal › Article › peer-review

Abstract

Traditional anticancer therapy faces major limitations due to the off-target toxicity of drugs. A specialized drug delivery system (DDS) has proven to be a potential approach for overcoming this barrier. Targeted delivery to cancer cells not only enhances the precision of drug localization but also minimizes adverse effects of the drug by further directing therapeutic agents selectively to their site of action inside specific intracellular organelles. Among various targets, folate receptors show a significantly higher level of expression in many cancer types, making them suitable for preclinical developments. Moreover, after this selective delivery of anticancer drugs to cancer cells, regulation of the intracellular trafficking process could also impact the efficacy of drug actions. This selective targeting of cancer cells and delivery of drugs to their sites of action could be achieved by using two different types of targeting ligands on the same DDS surface. Herein, we used a chitosan-based biopolymer, modified by cholesterol molecules using a simple chemical approach and installed dual ligands, folic acid (FA) and triphenylphosphine (TPP) for selective cancer cell targeting and further mitochondrial delivery of curcumin. Cellular uptake studies in KB cells, which overexpress folate receptors, using fluorescence microscopy and flow cytometry analysis confirmed that the targeted DDS has many-fold higher cellular uptake than the nontargeted DDS (without decoration of TPP) and the null DDS (without FA and TPP on its surface), respectively, which induced more cytotoxic effects on cancer cells. The developed chemical approach employed for polymer synthesis and ligand decoration is a simple, straightforward, and one-step process that generates a versatile and multifaceted DDS with the possibility to encapsulate a wide variety of drugs (hydrophobic, charged, small molecule, biomolecule drugs, etc.) and ligands for enhanced precision therapy.

Original language	English
Pages (from-to)	19668-19678
Number of pages	11
Journal	ACS Applied Nano Materials
Volume	8
Issue number	40
DOIs	https://doi.org/10.1021/acsanm.5c04231
State	Published - 10 Oct 2025
Externally published	Yes

Keywords

anticancer therapy
cancer cell targeting
drug delivery system
dual ligands
mitochondrial drug delivery
triphenylphosphine

ASJC Scopus subject areas

General Materials Science

Access to Document

10.1021/acsanm.5c04231

Cite this

Kishore, P., Barman, S., Dey, R., Jana, A., Ghosh, M., Bag, P., Ghatak, T., Maji, P. S., Ghosh, C., Mukherjee, N., Dutta Chowdhury, A., Ghatak, S., Mukherjee, R., Basu, A., Khan, A. H., Ghosh, S. K., Mandal, S., & Maity, A. R. (2025). Delivering Drugs to Cancer Cells and inside the Mitochondria Using a Dual-Ligand Installed Targeted Drug Delivery System. ACS Applied Nano Materials, 8(40), 19668-19678. https://doi.org/10.1021/acsanm.5c04231

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title = "Delivering Drugs to Cancer Cells and inside the Mitochondria Using a Dual-Ligand Installed Targeted Drug Delivery System",

abstract = "Traditional anticancer therapy faces major limitations due to the off-target toxicity of drugs. A specialized drug delivery system (DDS) has proven to be a potential approach for overcoming this barrier. Targeted delivery to cancer cells not only enhances the precision of drug localization but also minimizes adverse effects of the drug by further directing therapeutic agents selectively to their site of action inside specific intracellular organelles. Among various targets, folate receptors show a significantly higher level of expression in many cancer types, making them suitable for preclinical developments. Moreover, after this selective delivery of anticancer drugs to cancer cells, regulation of the intracellular trafficking process could also impact the efficacy of drug actions. This selective targeting of cancer cells and delivery of drugs to their sites of action could be achieved by using two different types of targeting ligands on the same DDS surface. Herein, we used a chitosan-based biopolymer, modified by cholesterol molecules using a simple chemical approach and installed dual ligands, folic acid (FA) and triphenylphosphine (TPP) for selective cancer cell targeting and further mitochondrial delivery of curcumin. Cellular uptake studies in KB cells, which overexpress folate receptors, using fluorescence microscopy and flow cytometry analysis confirmed that the targeted DDS has many-fold higher cellular uptake than the nontargeted DDS (without decoration of TPP) and the null DDS (without FA and TPP on its surface), respectively, which induced more cytotoxic effects on cancer cells. The developed chemical approach employed for polymer synthesis and ligand decoration is a simple, straightforward, and one-step process that generates a versatile and multifaceted DDS with the possibility to encapsulate a wide variety of drugs (hydrophobic, charged, small molecule, biomolecule drugs, etc.) and ligands for enhanced precision therapy.",

keywords = "anticancer therapy, cancer cell targeting, drug delivery system, dual ligands, mitochondrial drug delivery, triphenylphosphine",

author = "Purvi Kishore and Sourav Barman and Rimpa Dey and Ankita Jana and Malabika Ghosh and Pousali Bag and Tapas Ghatak and Maji, \{Partha Sona\} and Chitrita Ghosh and Nayana Mukherjee and \{Dutta Chowdhury\}, Ankan and Souvik Ghatak and Rupam Mukherjee and Arnab Basu and Khan, \{Ali Hossain\} and Ghosh, \{Surya K.\} and Sadananda Mandal and Maity, \{Amit Ranjan\}",

note = "Publisher Copyright: {\textcopyright} 2025 American Chemical Society",

year = "2025",

month = oct,

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doi = "10.1021/acsanm.5c04231",

language = "English",

volume = "8",

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Kishore, P, Barman, S, Dey, R, Jana, A, Ghosh, M, Bag, P, Ghatak, T, Maji, PS, Ghosh, C, Mukherjee, N, Dutta Chowdhury, A, Ghatak, S, Mukherjee, R, Basu, A, Khan, AH, Ghosh, SK, Mandal, S & Maity, AR 2025, 'Delivering Drugs to Cancer Cells and inside the Mitochondria Using a Dual-Ligand Installed Targeted Drug Delivery System', ACS Applied Nano Materials, vol. 8, no. 40, pp. 19668-19678. https://doi.org/10.1021/acsanm.5c04231

TY - JOUR

T1 - Delivering Drugs to Cancer Cells and inside the Mitochondria Using a Dual-Ligand Installed Targeted Drug Delivery System

AU - Kishore, Purvi

AU - Barman, Sourav

AU - Dey, Rimpa

AU - Jana, Ankita

AU - Ghosh, Malabika

AU - Bag, Pousali

AU - Ghatak, Tapas

AU - Maji, Partha Sona

AU - Ghosh, Chitrita

AU - Mukherjee, Nayana

AU - Dutta Chowdhury, Ankan

AU - Ghatak, Souvik

AU - Mukherjee, Rupam

AU - Basu, Arnab

AU - Khan, Ali Hossain

AU - Ghosh, Surya K.

AU - Mandal, Sadananda

AU - Maity, Amit Ranjan

PY - 2025/10/10

Y1 - 2025/10/10

N2 - Traditional anticancer therapy faces major limitations due to the off-target toxicity of drugs. A specialized drug delivery system (DDS) has proven to be a potential approach for overcoming this barrier. Targeted delivery to cancer cells not only enhances the precision of drug localization but also minimizes adverse effects of the drug by further directing therapeutic agents selectively to their site of action inside specific intracellular organelles. Among various targets, folate receptors show a significantly higher level of expression in many cancer types, making them suitable for preclinical developments. Moreover, after this selective delivery of anticancer drugs to cancer cells, regulation of the intracellular trafficking process could also impact the efficacy of drug actions. This selective targeting of cancer cells and delivery of drugs to their sites of action could be achieved by using two different types of targeting ligands on the same DDS surface. Herein, we used a chitosan-based biopolymer, modified by cholesterol molecules using a simple chemical approach and installed dual ligands, folic acid (FA) and triphenylphosphine (TPP) for selective cancer cell targeting and further mitochondrial delivery of curcumin. Cellular uptake studies in KB cells, which overexpress folate receptors, using fluorescence microscopy and flow cytometry analysis confirmed that the targeted DDS has many-fold higher cellular uptake than the nontargeted DDS (without decoration of TPP) and the null DDS (without FA and TPP on its surface), respectively, which induced more cytotoxic effects on cancer cells. The developed chemical approach employed for polymer synthesis and ligand decoration is a simple, straightforward, and one-step process that generates a versatile and multifaceted DDS with the possibility to encapsulate a wide variety of drugs (hydrophobic, charged, small molecule, biomolecule drugs, etc.) and ligands for enhanced precision therapy.

AB - Traditional anticancer therapy faces major limitations due to the off-target toxicity of drugs. A specialized drug delivery system (DDS) has proven to be a potential approach for overcoming this barrier. Targeted delivery to cancer cells not only enhances the precision of drug localization but also minimizes adverse effects of the drug by further directing therapeutic agents selectively to their site of action inside specific intracellular organelles. Among various targets, folate receptors show a significantly higher level of expression in many cancer types, making them suitable for preclinical developments. Moreover, after this selective delivery of anticancer drugs to cancer cells, regulation of the intracellular trafficking process could also impact the efficacy of drug actions. This selective targeting of cancer cells and delivery of drugs to their sites of action could be achieved by using two different types of targeting ligands on the same DDS surface. Herein, we used a chitosan-based biopolymer, modified by cholesterol molecules using a simple chemical approach and installed dual ligands, folic acid (FA) and triphenylphosphine (TPP) for selective cancer cell targeting and further mitochondrial delivery of curcumin. Cellular uptake studies in KB cells, which overexpress folate receptors, using fluorescence microscopy and flow cytometry analysis confirmed that the targeted DDS has many-fold higher cellular uptake than the nontargeted DDS (without decoration of TPP) and the null DDS (without FA and TPP on its surface), respectively, which induced more cytotoxic effects on cancer cells. The developed chemical approach employed for polymer synthesis and ligand decoration is a simple, straightforward, and one-step process that generates a versatile and multifaceted DDS with the possibility to encapsulate a wide variety of drugs (hydrophobic, charged, small molecule, biomolecule drugs, etc.) and ligands for enhanced precision therapy.

KW - anticancer therapy

KW - cancer cell targeting

KW - drug delivery system

KW - dual ligands

KW - mitochondrial drug delivery

KW - triphenylphosphine

UR - https://www.scopus.com/pages/publications/105018741911

U2 - 10.1021/acsanm.5c04231

DO - 10.1021/acsanm.5c04231

M3 - Article

AN - SCOPUS:105018741911

SN - 2574-0970

VL - 8

SP - 19668

EP - 19678

JO - ACS Applied Nano Materials

JF - ACS Applied Nano Materials

IS - 40

ER -

Delivering Drugs to Cancer Cells and inside the Mitochondria Using a Dual-Ligand Installed Targeted Drug Delivery System

Abstract

Keywords

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