Survivin Blockade Sensitizes Rhabdomyosarcoma Cells for Lysis by Fetal Acetylcholine Receptor–Redirected T Cells

Jia

J Biochem & Molecular Tox

2013

Arctigenin, a dibenzylbutyrolactone lignan, enhances cisplatin-mediated cell apoptosis in cancer cells. Here, we sought to investigate the effects of arctigenin on cisplatin-treated non-small-cell lung cancer (NSCLC) H460 cells. The 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assay and annexin-V/propidium iodide staining were performed to analyze the proliferation and apoptosis of H460 cells. Arctigenin dose-dependently suppressed cell proliferation and potentiated cell apoptosis, coupled with increased cleavage of caspase-3 and poly(ADP-ribose) polymerase. Moreover, arctigenin sensitized H460 cells to cisplatin-induced proliferation inhibition and apoptosis. Arctigenin alone or in combination with cisplatin had a significantly lower amount of survivin. Ectopic expression of survivin decreased cell apoptosis induced by arctigenin (P < 0.05) or in combination with cisplatin (P < 0.01). Moreover, arctigenin (P < 0.05) or in combination with cisplatin (P < 0.01) induced G1/G0 cell-cycle arrest. Our data provide evidence that arctigenin has a therapeutic potential in combina-tion with chemotherapeutic agents for NSLC.

Section: Discussionmentioning

confidence: 99%

Arctigenin Enhances Chemosensitivity to Cisplatin in Human Nonsmall Lung Cancer H460 Cells through Downregulation of Survivin Expression

Jia

J Biochem & Molecular Tox

2013

“…RNA isolation from unfixed thymoma tissue, thymocytes derived thereof, PBMCs, T-cell subsets, and B cells; cDNA synthesis; qRT-PCR (relative quantification was calculated using the ΔΔCt method with Glycerinaldehyd-3-phosphat-Dehydrogenase (GAPDH) standard: TaqMan; FAST SYBR Green; Applied Biosystems, Darmstadt, Germany), and western blot were performed as described. 13 Cytosolic and nuclear proteins were isolated using NE-PER Nuclear and Cytoplasmic Extraction Reagents (Thermoscientific, Karlsruhe, Germany). Mouse anti-cFLIP (G11 D16A8; Cell Signaling, Francfort, Germany), rabbit anti-p65 (C-20, sc-372; Abcam, UK ) , rabbit anti-ß-actin (New England Biolabs, Frankfurt, Germany), and PARP (poly (ADP ribose) polymerase (H-250) Santa Cruz, Heidelberg, Germany) were used for western blot.…”

Section: Patient Characteristics and Experimental Proceduresmentioning

confidence: 99%

“…Survival of PBMCs was measured by MTT assay (Sigma Aldrich, Munich Germany) 13 For apoptosis induction, 10 5 PBMCs from thymoma patients and blood donors were treated with 5–10 ng/mL FASLG (Sigma Aldrich, Germany) for 24 h, followed by MTT assay. FAS expression levels on PBMCs were quantified by flow cytometry, using FITC-conjugated mouse anti-human-CD95 (clone DX2; BD Pharmingen, Heidelberg Germany).…”

Section: Patient Characteristics and Experimental Proceduresmentioning

confidence: 99%

cFLIP overexpression in T cells in thymoma‐associated myasthenia gravis

Belharazem

Schalke

Gold³

et al. 2015

Ann Clin Transl Neurol

Self Cite

ObjectiveThe capacity of thymomas to generate mature CD4+ effector T cells from immature precursors inside the tumor and export them to the blood is associated with thymoma-associated myasthenia gravis (TAMG). Why TAMG(+) thymomas generate and export more mature CD4+ T cells than MG(−) thymomas is unknown.MethodsUnfixed thymoma tissue, thymocytes derived thereof, peripheral blood mononuclear cells (PBMCs), T-cell subsets and B cells were analysed using qRT-PCR and western blotting. Survival of PBMCs was measured by MTT assay. FAS-mediated apoptosis in PBMCs was quantified by flow cytometry. NF-κB in PBMCs was inhibited by the NF-κB-Inhibitor, EF24 prior to FAS-Ligand (FASLG) treatment for apoptosis induction.ResultsExpression levels of the apoptosis inhibitor cellular FLICE-like inhibitory protein (c-FLIP) in blood T cells and intratumorous thymocytes were higher in TAMG(+) than in MG(−) thymomas and non-neoplastic thymic remnants. Thymocytes and PBMCs of TAMG patients showed nuclear NF-κB accumulation and apoptosis resistance to FASLG stimulation that was sensitive to NF-κB blockade. Thymoma removal reduced cFLIP expression in PBMCs.InterpretationWe conclude that thymomas induce cFLIP overexpression in thymocytes and their progeny, blood T cells. We suggest that the stronger cFLIP overexpression in TAMG(+) compared to MG(−) thymomas allows for the more efficient generation of mature CD4+ T cells in TAMG(+) thymomas. cFLIP overexpression in thymocytes and exported CD4+ T cells of patients with TAMG might contribute to the pathogenesis of TAMG by impairing central and peripheral T-cell tolerance.

“…One Phase I trial that included mostly patients with bone sarcomas, but one patient with DSRCT, showed tolerability of HER2 CAR T cells 183. In solid tumor CAR T cell therapy, the tumor microenvironment seems to interfere with proper T cell function184 and this might also apply to sarcomas 179. New approaches incorporating immune-modulatory strategies, such as PD-1 or gamma delta T cells into CAR T cell therapeutic approaches,185–187 are being investigated.…”

Section: Immunotherapymentioning

confidence: 99%

Targeted therapy for soft tissue sarcomas in adolescents and young adults

Steppan

Pratilas

Loeb

2017

AHMT

Soft tissue sarcomas (STSs) are a heterogeneous group of tumors originating from the mesenchyme. Even though they affect individuals in all age groups, the prevalence of subtypes of STSs changes significantly from childhood through adolescence into adulthood. The mainstay of therapy is surgery, with or without the addition of chemotherapy and/or radiation therapy. These treatment modalities are associated, in many cases, with significant morbidity and, given the heterogeneity of tumor histologies encompassed by the term “STS”, have not uniformly improved outcomes. Moreover, some subgroups of STSs appear to be more, and others less, responsive to conventional chemotherapy agents. Over the last two decades, our understanding of the biology of STSs is slowly increasing, allowing for the development of more targeted therapies. We review the new treatment modalities that have been tested on patients with STSs, with a special focus on adolescents and young adults, a group of patients that is often underrepresented in clinical trials and has not received the dedicated attention it deserves, given the significant differences in biology and treatment response in comparison to children and adults.