CD30-targeted oncolytic viruses as novel therapeutic approach against classical Hodgkin lymphoma

Jds, Hanauer; Rengstl, Benjamin; Kleinlützum, Dina; Reul, Johanna; Pfeiffer, Anett; Friedel, Thorsten; Ic, Schneider; Newrzela, Sebastian; Ml, Hansmann; Buchholz, Christian J.; Muik, Alexander

doi:10.18632/oncotarget.24191

Cited by 19 publications

(9 citation statements)

References 43 publications

(60 reference statements)

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“…By exchanging the gfp marker gene against the prodrug convertase SCD encoding scd gene via the DNA fragment also containing the MeV N gene cassette by Mlu I/ SbfI (NEB), plasmid p(+)PolII-MV NSe -MMPA1-SCD(N)-E.01 was generated. The expression plasmid pCG-F-IRES-Puro allowing selection of MeV-F expression by coupling F mRNA to puromycin resistance was generated by blunt end insertion of the IRES-Puromycin cassette released from pH-HCD30-IP-LTR 41 via Spe I and Acc65 I 3′ to the F gene by linearization of pCG-F 42 using XbaI (NEB) and subsequent Klenow (NEB) digestion to generate blunt ends and allowing ligation. EGFRvIII sequence was obtained by RNA isolation from U87MG.ΔEGFR cells that express EGFRvIII as a transgene.…”

Section: Methodsmentioning

confidence: 99%

High-Affinity DARPin Allows Targeting of MeV to Glioblastoma Multiforme in Combination with Protease Targeting without Loss of Potency

Hanauer

Koch

Lauer

et al. 2019

Molecular Therapy - Oncolytics

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Measles virus (MeV) is naturally cytolytic by extensive cell-to-cell fusion. Vaccine-derived MeV is toxic for cancer cells and is clinically tested as oncolytic virus. To combine the potential of MeV with enhanced safety, different targeting strategies have been described. We generated a receptor-targeted MeV by using receptor-blind viral attachment protein genetically fused to designed ankyrin repeat protein (DARPin) binding domains specific for the epidermal growth factor receptor (EGFR). To reduce on-target toxicity for EGFR+ healthy cells, we used an engineered viral fusion protein activatable by tumor-associated matrix metalloproteases (MMPs) for additional protease targeting. The dual-targeted virus replicated exclusively on EGFR+/MMP+ tumor cells but was safe on healthy EGFR+ target cells, primary human keratinocytes. Nevertheless, glioblastoma and other tumor cells were efficiently killed by all targeted viruses, although replication and oncolysis were slower for protease-targeted MeV. In vivo, efficacy of EGFR-targeted MeV was virtually unimpaired, whereas also dual-targeted MeV showed significant intra-tumoral spread and efficacy and could be armed with a prodrug convertase. The use of DARPin-domains resulted in potent EGFR-targeted MeV and for the first time effective dual retargeting of an oncolytic virus, further enhancing tumor selectivity. Together with powerful cell-toxic genes, the application as highly tumor-specific platform is promising.

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Section: Methodsmentioning

confidence: 99%

High-Affinity DARPin Allows Targeting of MeV to Glioblastoma Multiforme in Combination with Protease Targeting without Loss of Potency

Hanauer

Koch

Lauer

et al. 2019

Molecular Therapy - Oncolytics

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“…VSV is an enveloped virus of size 70 × 200 nm belonging to the Rhabdoviridae family containing an 11 kb single-stranded-RNA of negative sense 94 . VSV in particular is an attractive vector because of (1) its effectiveness against a variety of tumor models,95, 96, 97, 98, 99, 100, 101, 102 including leukemia 103 and lymphoma, 104 and (2) its sensitivity to type I IFNs, an innate immune mechanism found in normal cells but not in tumor cells, thus making the virus tumor selective and able to boost CD8 T cell responses 105, 106. In clinical trials, recombinant VSV expressing IFNβ has been tested against refractory multiple myeloma, acute myeloid leukemia, T cell lymphoma (ClinicalTrials.gov: NCT03017820) and refractory hepatocellular carcinoma (ClinicalTrials.gov: NCT01628640).…”

Section: Main Textmentioning

confidence: 99%

Oncolytic Viruses and Immune Checkpoint Inhibition: The Best of Both Worlds

Sivanandam

LaRocca

Chen

et al. 2019

Molecular Therapy - Oncolytics

115

113

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Cancer immunotherapy and the emergence of immune checkpoint inhibitors have markedly changed the treatment paradigm for many cancers. They function to disrupt cancer cell evasion of the immune response and activate sustained anti-tumor immunity. Oncolytic viruses have also emerged as an additional therapeutic agent for cancer treatment. These viruses are designed to target and kill tumor cells while leaving the normal cells unharmed. As part of this process, oncolytic virus infection stimulates anti-cancer immune responses that augment the efficacy of checkpoint inhibition. These viruses have the capability of transforming a "cold" tumor microenvironment with few immune effector cells into a "hot" environment with increased immune cell and cytokine infiltration. For this reason, there are multiple ongoing clinical trials that combine oncolytic virotherapy and immune checkpoint inhibitors. This review will detail the key oncolytic viruses in preclinical and clinical studies and highlight the results of their testing with checkpoint inhibitors. CTLA-4 CTLA-4, also known as CD152, is an inhibitory molecule on the surface of activated T cells 12 that inhibits the binding of B7 to CD28. 13 Its mechanism functions to halt the initial stage of naive T cell activation in the lymph nodes and results in decreased T cell responses. 14 Anti-CTLA-4 antibodies are designed to block

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“…The best studied oncolytic rhabdovirus Vesicular Stomatitis Virus (VSV) uses the low-density lipoprotein (LDL) receptor for cell entry, allowing VSV to infect nearly all cell types and cause lytic infection in a wide variety of permissive cells (57). Oncolytic VSV cell entry has been made tumor selective through retargeting strategies, involving replacing the VSV G with a more selective entry G as the measles F and H (hemagglutinin) proteins (58), receptor targeted measles H and F proteins (59,60), the lymphocytic choriomeningitis virus WE54-strain glycoprotein (LCMV-GP) (61) and Lassa virus G (62).…”

Section: Ovs In Clinical Developmentmentioning

confidence: 99%

The emerging role of oncolytic virus therapy against cancer

Russell¹,

Peng

2018

Chin. Clin. Oncol.

109

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This review discusses current clinical advancements in oncolytic viral therapy, with a focus on the viral platforms approved for clinical use and highlights the benefits each platform provides. Three oncolytic viruses (OVs), an echovirus, an adenovirus, and a herpes simplex-1 virus, have passed governmental regulatory approval in Latvia, China, and the USA and EU. Numerous other recombinant viruses from diverse families are in clinical testing in cancer patients and we highlight the design features of selected examples, including adenovirus, herpes simplex virus, measles virus, retrovirus, reovirus, vaccinia virus, vesicular stomatitis virus. Lastly, we provide thoughts on the path forward for this rapidly expanding field especially in combination with immune modulating drugs.

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CD30-targeted oncolytic viruses as novel therapeutic approach against classical Hodgkin lymphoma

Cited by 19 publications

References 43 publications

High-Affinity DARPin Allows Targeting of MeV to Glioblastoma Multiforme in Combination with Protease Targeting without Loss of Potency

High-Affinity DARPin Allows Targeting of MeV to Glioblastoma Multiforme in Combination with Protease Targeting without Loss of Potency

Oncolytic Viruses and Immune Checkpoint Inhibition: The Best of Both Worlds

The emerging role of oncolytic virus therapy against cancer

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