2007
DOI: 10.1084/jem.20042592082307c
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Sustained expansion of NKT cells and antigen-specific T cells after injection of α-galactosyl-ceramide loaded mature dendritic cells in cancer patients

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Cited by 79 publications
(120 citation statements)
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“…patients with various cancers [39], adult and pediatric acute versus chronic asthmatics, untreated or on various treatments [40][41][42][43][44][45]) and their various tissues, as well as intervening therapeutically. Given that several approaches to exploit iNKT cells have entered clinical trials [46,47], development of such a selective reagent seems timely. …”
Section: Discussionmentioning
confidence: 99%
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“…patients with various cancers [39], adult and pediatric acute versus chronic asthmatics, untreated or on various treatments [40][41][42][43][44][45]) and their various tissues, as well as intervening therapeutically. Given that several approaches to exploit iNKT cells have entered clinical trials [46,47], development of such a selective reagent seems timely. …”
Section: Discussionmentioning
confidence: 99%
“…(A) Histograms of Va24, Vb11, and 6B11 expression as determined for a TCR-negative Jurkat cell subline transfected to transiently express iNKT Va24Ja18 and Vb11 TCR, as previously described for other CD1-reactive T cells [31]. (B) Liver mononuclear cells from human invariant Va24Ja18 transgenic mice [46] or C57BL/6 wild-type mice were specifically stained with 6B11-biotin or Va24-biotin and fluorescent streptavidin and otherwise with mouse-specific directly conjugated mAb as shown. Note that 6B11 identified high-and low-level expressing transgenic iNKT, whereas Va24 was uniformly positive.…”
Section: B11 Is Highly Specific For Inkt Subsets In Pbmcmentioning
confidence: 99%
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“…Numerical and functional iNKT cell deficiencies have been reported in a number of human diseases [189][190][191][192]. These findings led to clinical trials in humans for cancer involving the adoptive transfer of ex vivo expanded autologous DC, pulsed with a-GC, in the absence or presence of expanded iNKT cells [193][194][195]. Although these treatments were well-tolerated and resulted in the generation of antitumor CD4 + and CD8 + T cell responses, clinical responses have been limited and future refinements are required to optimize the generation of efficient antitumor immunity.…”
Section: Other Unconventional T Cells Bridging Innate and Adaptive Immentioning
confidence: 99%
“…Even more, other unconventional T cell subsets may drive similar reactions, albeit in response to different stimuli and in different anatomical contexts, arguing for a general role of innate T cell subsets as natural adjuvants to promote protective immune responses. In analogy to the exploitation of iNKT cells in the clinic [193][194][195]223,224], approaches specifically targeting Vc9/Vd2 T cells may have a similar potential as vaccine adjuvant, to boost immune responses against pathogens and tumors and to modulate autoimmune responses.…”
Section: Innate Regulation Of Adaptive Immune Responses: Vd2 + Versusmentioning
confidence: 99%