Mechanisms of Oncolytic Virus Targeting Tumor Cells

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Mechanisms of Oncolytic Virus Targeting Tumor Cells (Resource:https://www.creative-biolabs.com/oncolytic-virus/mechanisms-of-oncolytic-virustargeting-tumor-cells.htm)

Oncolytic viruses (OVs) are viral strains that can infect and kill malignant cells (oncolysis) while sparing their normal counterparts. Some viruses demonstrate a natural ability to target cancer cells selectively and more efficiently than normal cells. Cancer cells have several distinct hallmarks that separate them from normal cells: sustained growth signals, insensitivity to anti-growth signals, evasion of apoptosis, increased angiogenesis, cell immortality, and invasion/metastasis. OVs utilize several mechanisms to enter cancer cellsďźŒCreative Biolabs has summarized those regulations as following. 1. Abnormal cell receptors Cancer cells have been shown to overexpress selected surface receptors, by which viruses may selectively bind to and infect cancer cells. 2. Aberrant signaling pathways In fact, some viruses naturally exploit the aberrant signaling pathways that maintain sustained cancer growth in order to selectively infect and replicate within cancer cells as opposed to normal cells. 3. The hypoxic environment The rapid proliferation of tumor cells results in the majority of solid tumor tissues in a hypoxic state. Fortunately, some oncolytic viruses can selectively infect tumor tissues in a low oxygen environment.

Abnormal cell receptors Some viruses can enter cells through one or more receptors and some of which can promote the entry of more than one type of virus. Some viruses, like Newcastle disease virus (NDV), vaccinia virus (VV), and stomatitis virus vesicul, use endocytosis through membrane fusion and syncytia formation to enter cells. Certain oncolytic viruses, such as Seneca valley virus and reovirus, are known to preferentially target cancer cells but the cell surface receptor for entry has not been identified. Many of the oncolytic viruses currently in the clinic have a natural tropism for cell surface proteins aberrantly expressed by cancer cells.


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