Mesenchymal stem cells: A new platform for targeting suicide genes in cancer

Tehrani, Rana Moradian; Verdi, Javad; Noureddini, Mahdi; Salehi, Roya; Salarinia, Reza; Mosalaei, Meysam; Simonian, Miganosh; Alani, Behrang; Ghiasi, Moosa Rahimi; Jaafari, Mahmoud Reza; Mirzaei, Hamed

doi:10.1002/jcp.26094

Cited by 64 publications

(36 citation statements)

References 187 publications

(222 reference statements)

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“…can easily be isolated and expanded in large amounts from adult mammals without major ethical concerns; (b.) undergo targeted tropism towards growing tumors; (c.) migrate deep into the tumor microenvironment; (d.) differentiate into cells of the tumor stroma (cancer‐associated fibroblasts, pericytes and endothelial cells); (e.) have low immunogenicity and can potentially avoid immune rejection …”

Section: Introductionmentioning

confidence: 99%

Treatment of advanced gastrointestinal cancer with genetically modified autologous mesenchymal stem cells: Results from the phase 1/2 TREAT‐ME‐1 trial

Einem¹,

Guenther

Volk

et al. 2019

Intl Journal of Cancer

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TREAT‐ME‐1, a Phase 1/2 open‐label multicenter, first‐in‐human, first‐in‐class trial, evaluated the safety, tolerability and efficacy of treatment with genetically modified autologous mesenchymal stromal cells (MSC), MSC_ apceth_101, in combination with ganciclovir in patients with advanced gastrointestinal adenocarcinoma. Immunological and inflammatory markers were also assessed. All patients (3 in Phase 1; 7 in Phase 2) received three treatment cycles of MSC_apceth_101 at one dose level on Day 0, 7, and 14 followed by ganciclovir administration according to the manufacturer's instructions for 48─72 h after MSC_apceth_101 injection. Ten patients were treated with a total dose of 3.0 x 106 cells/kg MSC_apceth_101. 36 adverse events and six serious adverse events were reported. Five patients achieved stable disease (change in target lesions of −2 to +28%). For all patients, the median time to progression was 1.8 months (95% CI: 0.5, 3.9 months). Median overall survival could not be estimated as 8/10 patients were still alive at the end of the study (1 year) and therefore censored. Post‐study observation of patients showed a median overall survival of 15.6 months (ranging from 2.2─27.0 months). Treatment with MSC_apceth_101 and ganciclovir did not induce a consistent increase or decrease in levels of any of the tumor markers analyzed. No clear trends in the immunological markers assessed were observed. MSC_apceth_101 in combination with ganciclovir was safe and tolerable in patients with advanced gastrointestinal adenocarcinoma, with preliminary signs of efficacy in terms of clinical stabilization of disease.

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Section: Introductionmentioning

confidence: 99%

Treatment of advanced gastrointestinal cancer with genetically modified autologous mesenchymal stem cells: Results from the phase 1/2 TREAT‐ME‐1 trial

Einem¹,

Guenther

Volk

et al. 2019

Intl Journal of Cancer

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“…In vivo studies have repeatedly shown that MSCs are trapped after intravenous injection [ 82 , 83 ]. Many existing methods are used to modify MSCs and the most commonly used are genetically modified MSCs [ 84 , 85 ]. The cells can transport the agents into the tumor microenvironment and greatly reduce the immune reaction in vivo through high concentration anticancer agents target tumor site.…”

Section: Effect Of Mscs On Colon Cancersmentioning

confidence: 99%

The Dynamic Roles of Mesenchymal Stem Cells in Colon Cancer

Wang

Miao

Yang

et al. 2018

Canadian Journal of Gastroenterology and Hepatology

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Colon cancer is still one of the most common causes of cancer in human and is characterized by lymphocyte infiltrates and originates from the epithelial cells found in the lining of colon or rectum of the gastrointestinal tract. Mesenchymal stem cells (MSCs) are composed of the multipotent stem cell group of stroma and can be differentiated as various cell lineages, such as fibroblasts, osteoblasts, and adipocytes. MSCs provide mechanical and structural support and have potential functions during tumor growth and metastasis. The efficacy of MSC-based therapies is partly dependent on the migration and homing of MSCs to tumors and metastatic sites. However, their migratory and engraftment potential is poorly understood. In this review, the characteristics and mechanisms of MSC's dynamic interaction with colon cancer were summarized, particularly the potential functions of MSCs on colon cancer, including its role in improving tumor growth and as a potential candidate for tumor therapy. Understanding MSC homing provides new insights into the manipulation of MSC and the improvement of their efficacy for colon cancer therapy.

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“…Viral vectors are particularly appealing because they can enable high transduction efficiency and, depending on the type of virus used, can deliver long-term stable transgene expression. The safety of cell-based therapy with the use of viral vectors is a crucial issue that has not been resolved yet, but advances in vector design have helped towards this direction ( 23 , 95 ). For example, MSCs genetically modified to express VEGF have been shown to enhance the cardioprotective effects of MSCs followed by angiogenesis effects for the treatment of acute MI, whereas Akt gene- or heme oxygenase-1 ( HO-1 ) gene-modified MSCs have been shown to dramatically improve ischemic cardiac function and MSC viability and prevent ventricular remodeling and apoptosis of cardiomyocytes and endothelial cells, thus restoring the function of infarcted hearts ( 91 , 96 – 98 ).…”

Section: Genetically-modified Stem Cells In Treatment Of Human Dismentioning

confidence: 99%

Genetically‑modified stem cells in treatment of human diseases: Tissue kallikrein (KLK1)‑based targeted therapy (Review)

et al. 2018

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The tissue kallikrein-kinin system (KKS) is an endogenous multiprotein metabolic cascade which is implicated in the homeostasis of the cardiovascular, renal and central nervous system. Human tissue kallikrein (KLK1) is a serine protease, component of the KKS that has been demonstrated to exert pleiotropic beneficial effects in protection from tissue injury through its anti-inflammatory, anti-apoptotic, anti-fibrotic and anti-oxidative actions. Mesenchymal stem cells (MSCs) or endothelial progenitor cells (EPCs) constitute populations of well-characterized, readily obtainable multipotent cells with special immunomodulatory, migratory and paracrine properties rendering them appealing potential therapeutics in experimental animal models of various diseases. Genetic modification enhances their inherent properties. MSCs or EPCs are competent cellular vehicles for drug and/or gene delivery in the targeted treatment of diseases. KLK1 gene delivery using adenoviral vectors or KLK1 protein infusion into injured tissues of animal models has provided particularly encouraging results in attenuating or reversing myocardial, renal and cerebrovascular ischemic phenotype and tissue damage, thus paving the way for the administration of genetically modified MSCs or EPCs with the human tissue KLK1 gene. Engraftment of KLK1-modified MSCs and/or KLK1-modified EPCs resulted in advanced beneficial outcome regarding heart and kidney protection and recovery from ischemic insults. Collectively, findings from pre-clinical studies raise the possibility that tissue KLK1 may be a novel future therapeutic target in the treatment of a wide range of cardiovascular, cerebrovascular and renal disorders.

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Mesenchymal stem cells: A new platform for targeting suicide genes in cancer

Cited by 64 publications

References 187 publications

Treatment of advanced gastrointestinal cancer with genetically modified autologous mesenchymal stem cells: Results from the phase 1/2 TREAT‐ME‐1 trial

Treatment of advanced gastrointestinal cancer with genetically modified autologous mesenchymal stem cells: Results from the phase 1/2 TREAT‐ME‐1 trial

The Dynamic Roles of Mesenchymal Stem Cells in Colon Cancer

Genetically‑modified stem cells in treatment of human diseases: Tissue kallikrein (KLK1)‑based targeted therapy (Review)

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