2009
DOI: 10.1016/j.imlet.2009.08.010
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LIGHT protein suppresses tumor growth by augmentation of immune response

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Cited by 9 publications
(9 citation statements)
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References 35 publications
(49 reference statements)
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“…LIGHT protein was generated by truncation of the N-terminal 65 amino acids, which removes the cytoplasmic and transmembrane domains. We have confirmed that non-glycosylated LIGHT expressed in E. coli had the same bioactivity and receptor binding capacity compared to LIGHT expressed in mammalian cells, although LIGHT has a single N-linked glycosylation site (Asn102) [12]. So, in this study, we manufactured LIGHT mutants in E. coli as previously described [12].…”
Section: Receptor Selectivity Of Light Mutantsupporting
confidence: 56%
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“…LIGHT protein was generated by truncation of the N-terminal 65 amino acids, which removes the cytoplasmic and transmembrane domains. We have confirmed that non-glycosylated LIGHT expressed in E. coli had the same bioactivity and receptor binding capacity compared to LIGHT expressed in mammalian cells, although LIGHT has a single N-linked glycosylation site (Asn102) [12]. So, in this study, we manufactured LIGHT mutants in E. coli as previously described [12].…”
Section: Receptor Selectivity Of Light Mutantsupporting
confidence: 56%
“…Therefore, we expect that LIGHT might have the potential for superior therapeutic efficiency in immunotherapy for various cancers, and also the potential for marked anti-tumor activity in restraining metastasis and recrudescence. In fact, we and others have also demonstrated the usefulness of LIGHT for cancer immunotherapy [7,[9][10][11][12][13]. Therefore, LIGHT has recently attracted a great deal of attention as a superior agent for cytokine-based cancer immunotherapy for the eradication of not only local, but also disseminated, metastases.…”
Section: Introductionmentioning
confidence: 94%
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