FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W185339859> ?p ?o ?g. }

• W185339859 endingPage "301" @default.
• W185339859 startingPage "287" @default.
• W185339859 abstract "An adoptive therapy model has been utilized to examine the requirements for T cells to promote eradication of a disseminated, retrovirus-induced, syngeneic leukemia. Complete tumor elimination required that the transferred T cells proliferate in the host and mediate an anti-tumor effect for more than 30 days. Non-cytolytic L3T4+ T helper (Th) cells were capable of eliminating disseminated tumor without the participation of Lyt-2+ cytotoxic T cells (Tc). Purified or cloned Lyt-2+ T cells were also effective in therapy, but required the concurrent administration of either L3T4+ Th or interleukin 2 (IL-2) for optimal efficacy. L3T4+ Th appear to function via secretion of lymphokines that activate macrophages to a cytotoxic state. Lyt-2+ Tc, in addition to direct cytotoxicity, may mediate tumor eradication in part by secretion of lymphokines that activate in vivo tumoricidal macrophages. These studies suggested that the reported efficacy of individual T cell subsets in therapy of particular tumors might not reflect resistance or susceptibility to a cytotoxic effector mechanism, but rather the efficiency with which a T cell subset is activated by the tumor and/or recognizes the tumor antigen. Methods were developed to independently assess the activation and proliferation requirements of each subset. L3T4+ Th required that macrophages degrade tumor antigens in lysosomes and present the antigens in the context of class II molecules, and produced IL-2 and IL-4 as endogenous growth factors. By contrast, Lyt-2+ T cells recognized the tumor directly, required macrophages only to produce IL-1 for activation, and produced IL-2 but not IL-4 as an endogenous growth factor. The ability of T cell subsets to recognize the distinct retroviral tumor antigens expressed on FBL leukemia was assessed using cell lines or recombinant vaccinia viruses transfected with selected retroviral genes. Highly selective antigen recognition was detected, with Lyt-2+ Tc cells recognizing products of gag but not envelope genes, and L3T4+ Th recognizing envelope but not gag products. The results suggest that even complex unique tumor antigens may elicit only limited host T cell responses." @default.
• W185339859 created "2016-06-24" @default.
• W185339859 creator A5007551071 @default.
• W185339859 creator A5022298525 @default.
• W185339859 creator A5030463228 @default.
• W185339859 creator A5038003907 @default.
• W185339859 creator A5064774655 @default.
• W185339859 creator A5087281332 @default.
• W185339859 date "1988-01-01" @default.
• W185339859 modified "2023-10-02" @default.
• W185339859 title "Requirements for T cell recognition and elimination of retrovirally-transformed cells." @default.
• W185339859 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/2479634" @default.
• W185339859 hasPublicationYear "1988" @default.
• W185339859 type Work @default.
• W185339859 sameAs 185339859 @default.
• W185339859 citedByCount "3" @default.
• W185339859 crossrefType "journal-article" @default.
• W185339859 hasAuthorship W185339859A5007551071 @default.
• W185339859 hasAuthorship W185339859A5022298525 @default.
• W185339859 hasAuthorship W185339859A5030463228 @default.
• W185339859 hasAuthorship W185339859A5038003907 @default.
• W185339859 hasAuthorship W185339859A5064774655 @default.
• W185339859 hasAuthorship W185339859A5087281332 @default.
• W185339859 hasConcept C147483822 @default.
• W185339859 hasConcept C154317977 @default.
• W185339859 hasConcept C185592680 @default.
• W185339859 hasConcept C202751555 @default.
• W185339859 hasConcept C203014093 @default.
• W185339859 hasConcept C2776090121 @default.
• W185339859 hasConcept C2776662205 @default.
• W185339859 hasConcept C2777371288 @default.
• W185339859 hasConcept C2777701055 @default.
• W185339859 hasConcept C2778326572 @default.
• W185339859 hasConcept C49382859 @default.
• W185339859 hasConcept C502942594 @default.
• W185339859 hasConcept C55493867 @default.
• W185339859 hasConcept C86803240 @default.
• W185339859 hasConcept C8891405 @default.
• W185339859 hasConcept C90375314 @default.
• W185339859 hasConceptScore W185339859C147483822 @default.
• W185339859 hasConceptScore W185339859C154317977 @default.
• W185339859 hasConceptScore W185339859C185592680 @default.
• W185339859 hasConceptScore W185339859C202751555 @default.
• W185339859 hasConceptScore W185339859C203014093 @default.
• W185339859 hasConceptScore W185339859C2776090121 @default.
• W185339859 hasConceptScore W185339859C2776662205 @default.
• W185339859 hasConceptScore W185339859C2777371288 @default.
• W185339859 hasConceptScore W185339859C2777701055 @default.
• W185339859 hasConceptScore W185339859C2778326572 @default.
• W185339859 hasConceptScore W185339859C49382859 @default.
• W185339859 hasConceptScore W185339859C502942594 @default.
• W185339859 hasConceptScore W185339859C55493867 @default.
• W185339859 hasConceptScore W185339859C86803240 @default.
• W185339859 hasConceptScore W185339859C8891405 @default.
• W185339859 hasConceptScore W185339859C90375314 @default.
• W185339859 hasLocation W1853398591 @default.
• W185339859 hasOpenAccess W185339859 @default.
• W185339859 hasPrimaryLocation W1853398591 @default.
• W185339859 hasRelatedWork W1517459791 @default.
• W185339859 hasRelatedWork W1606500885 @default.
• W185339859 hasRelatedWork W167975574 @default.
• W185339859 hasRelatedWork W185339859 @default.
• W185339859 hasRelatedWork W1986580574 @default.
• W185339859 hasRelatedWork W1999068360 @default.
• W185339859 hasRelatedWork W2014063735 @default.
• W185339859 hasRelatedWork W2057586436 @default.
• W185339859 hasRelatedWork W2087981636 @default.
• W185339859 hasRelatedWork W2103739833 @default.
• W185339859 hasVolume "19" @default.
• W185339859 isParatext "false" @default.
• W185339859 isRetracted "false" @default.
• W185339859 magId "185339859" @default.
• W185339859 workType "article" @default.