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Characterization of patient-derived bone marrow human mesenchymal stem cells as oncolytic virus carriers for the treatment of glioblastoma. | LitMetric

AI Article Synopsis

  • The study investigates the use of bone marrow-derived human mesenchymal stem cells (BM-hMSCs) from glioma patients who have undergone marrow-toxic chemotherapy as carriers for an oncolytic virus called Delta-24-RGD, which targets and kills glioma cells.
  • Five patients with recurrent malignant glioma were enrolled, and their BM-hMSCs were cultured and shown to have similar properties to those from healthy donors, including the ability to differentiate into different cell types.
  • The findings indicate that the patient-derived BM-hMSCs effectively delivered Delta-24-RGD in preclinical models, significantly improving survival rates in mice with gliomas, suggesting potential for clinical application.

Article Abstract

Objective: Delta-24-RGD is an oncolytic adenovirus that is capable of replicating in and killing human glioma cells. Although intratumoral delivery of Delta-24-RGD can be effective, systemic delivery would improve its clinical application. Bone marrow-derived human mesenchymal stem cells (BM-hMSCs) obtained from healthy donors have been investigated as virus carriers. However, it is unclear whether BM-hMSCs can be derived from glioma patients previously treated with marrow-toxic chemotherapy or whether such BM-hMSCs can deliver oncolytic viruses effectively. Herein, the authors undertook a prospective clinical trial to determine the feasibility of obtaining BM-hMSCs from patients with recurrent malignant glioma who were previously exposed to marrow-toxic chemotherapy.

Methods: The authors enrolled 5 consecutive patients who had been treated with radiation therapy and chemotherapy. BM aspirates were obtained from the iliac crest and were cultured to obtain BM-hMSCs.

Results: The patient-derived BM-hMSCs (PD-BM-hMSCs) had a morphology similar to that of healthy donor-derived BM-hMSCs (HD-BM-hMSCs). Flow cytometry revealed that all 5 cell lines expressed canonical MSC surface markers. Importantly, these cultures could be made to differentiate into osteocytes, adipocytes, and chondrocytes. In all cases, the PD-BM-hMSCs homed to intracranial glioma xenografts in mice after intracarotid delivery as effectively as HD-BM-hMSCs. The PD-BM-hMSCs loaded with Delta-24-RGD (PD-BM-MSC-D24) effectively eradicated human gliomas in vitro. In in vivo studies, intravascular administration of PD-BM-MSC-D24 increased the survival of mice harboring U87MG gliomas.

Conclusions: The authors conclude that BM-hMSCs can be acquired from patients previously treated with marrow-toxic chemotherapy and that these PD-BM-hMSCs are effective carriers for oncolytic viruses.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10193507PMC
http://dx.doi.org/10.3171/2021.3.JNS203045DOI Listing

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