Formulation for the Targeted Delivery of a Vaccine Strain of Oncolytic Measles Virus (OMV) in Hyaluronic Acid Coated Thiolated Chitosan as a Green Nanoformulation for the Treatment of Prostate Cancer: A Viro-Immunotherapeutic Approach

Faiza Naseer; Tahir Ahmad; Kousain Kousar; Salik Kakar; Rabia Gul; Sadia Anjum; Usman Shareef

doi:10.2147/IJN.S386560

Formulation for the Targeted Delivery of a Vaccine Strain of Oncolytic Measles Virus (OMV) in Hyaluronic Acid Coated Thiolated Chitosan as a Green Nanoformulation for the Treatment of Prostate Cancer: A Viro-Immunotherapeutic Approach

Int J Nanomedicine. 2023 Jan 9:18:185-205. doi: 10.2147/IJN.S386560. eCollection 2023.

Authors

Faiza Naseer^{1

2}, Tahir Ahmad¹, Kousain Kousar¹, Salik Kakar³, Rabia Gul², Sadia Anjum⁴, Usman Shareef²

Affiliations

¹ Industrial Biotechnology, Atta-ur-Rehman School of Applied Biosciences, National University of Science and Technology, Islamabad, Pakistan.
² Shifa College of Pharmaceutical Sciences, Shifa Tameer e Millat University, Islamabad, Pakistan.
³ Healthcare Biotechnology, Atta-ur-Rehman School of Applied Biosciences, National University of Science and Technology, Islamabad, Pakistan.
⁴ Department of Biology, University of Hail, Hail, Saudia Arabia.

Abstract

Background: Oncolytic viruses are reported as dynamite against cancer treatment nowadays.

Methodology: In the present work, a live attenuated oral measles vaccine (OMV) strain was used to formulate a polymeric surface-functionalized ligand-based nanoformulation (NF). OMV (half dose: not less than 500 TCID units; 0.25 mL) was encapsulated in thiolated chitosan and outermost coating with hyaluronic acid by ionic gelation method characterizing parameters was performed.

Results and discussion: CD44 high expression was confirmed in prostatic adenocarcinoma (PRAD) by GEPIA which extracted data of normal and cancer tissue from GTEx and TCGA. Bioinformatics tools confirmed the viral hemagglutinin capsid protein interaction with human Caspase-I, NLRP3, and TNF-α and viral fusion protein interaction with COX-II and Caspase-I after successful delivery of MV encapsulated in NFs due to high affinity of hyaluronic acid with CD44 on the surface of prostate cancer cells. Particle size = 275.6 mm, PDI = 0.372, and ±11.5 zeta potential were shown by zeta analysis, while the thiolated group in NFs was confirmed by FTIR and Raman analysis. SEM and XRD showed a spherical smooth surface and crystalline nature, respectively, while TEM confirmed virus encapsulation within nanoparticles, which makes it very useful in targeted virus delivery systems. The virus was released from NFs in a sustained but continuous release pattern till 48 h. The encapsulated virus titer was calculated as 2.34×107 TCID50/mL units, which showed syncytia formation on post-day infection 7. Multiplicities of infection 0.1, 0.5, 1, 3, 5, 10, 15, and 20 of HA-coated OMV-loaded NFs as compared to MV vaccine on PC3 was inoculated with IC50 of 5.1 and 3.52, respectively, and growth inhibition was seen after 72 h via MTT assay which showed apoptotic cancer cell death.

Conclusion: Active targeted, efficacious, and sustained delivery of formulated oncolytic MV is a potent moiety in cancer treatment at lower doses with safe potential for normal prostate cells.

Keywords: controlled release; green synthesis; immunotherapeutic agent; in vitro studies; oncolytic activity; oncolytic measles virus; prostate cancer; targeted virus/drug delivery system; thiolated chitosan; tumour targeting; vaccine-based nanoformulation.

MeSH terms

Caspases
Chitosan* / chemistry
Humans
Hyaluronic Acid
Immunotherapy
Male
Measles virus / genetics
Nanoparticles* / chemistry
Oncolytic Viruses*
Prostatic Neoplasms* / pathology
Prostatic Neoplasms* / therapy
Vaccines*

Substances

Chitosan
Hyaluronic Acid
Vaccines
Caspases