Hepatic interleuklin 15 (IL-15) expression: implications for local NK/NKT cell homeostasis and development

Golden-Mason, Lucy; Kelly, Anna M; Doherty, Derek G.; Traynor, O.; McEntee, Gerry; Kelly, Jacinta; Hegarty, John E.; O’Farrelly, Cliona

doi:10.1111/j.1365-2249.2004.02586.x

Cited by 69 publications

(75 citation statements)

References 37 publications

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“…30,38,39 This may be important in the modulation of the immune response by the liver because Kupffer cells are a rich source of IL-15. 40,41 Thus, the liver can provide an environment for NK cells in which they can selectively eliminate colon and gastric carcinoma cells that express Hsp70 on their surfaces. The better overall survival demonstrated by our Kaplan-Meier analyses may reflect NK cell-mediated killing of tumor cells as they transit the liver.…”

Section: Discussionmentioning

confidence: 99%

Patient survival by Hsp70 membrane phenotype

Pfister

Radons

Busch

et al. 2007

Cancer

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BACKGROUNDHeat shock proteins (HSPs) play important roles in tumor immunity. The authors prospectively investigated the correlation between the tumor‐specific Hsp70 membrane expression as an independent clinicopathological marker and overall survival in tumor entities that differ in their route of metastasis.METHODSHsp70 membrane expression was examined by flow cytometry in 58 colon, 19 gastric, 54 lower rectal carcinoma, and 19 squamous cell carcinoma specimens and the corresponding normal tissues at time of first diagnosis. Kaplan‐Meier survival curves were analyzed to determine the relation of Hsp70 expression to the patients' prognosis.RESULTSAn Hsp70 membrane‐positive phenotype was found in 40% (colon), 37% (gastric), 43% (lower rectal), and 42% (squamous cell) of the analyzed tumor specimens. None of the corresponding normal tissues was found to be Hsp70 membrane‐positive. In patients with colon (P = .032) and gastric (P = .045) carcinomas, an Hsp70 membrane expression correlated significantly with an improved overall survival; a negative association was seen in lower rectal (P = .085) and squamous cell carcinoma (P = .048).CONCLUSIONSThe authors hypothesized that differing relations between surface expression of Hsp70 on tumor cells and clinical outcomes may reflect differences in the route of metastases. Colon and gastric carcinomas metastasize into the liver where hepatic natural killer cells may have the capacity to recognize and kill Hsp70 membrane‐positive tumor cells and thus account for a better overall survival. Cancer 2007; 110:926–35. © 2007 American Cancer Society.

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Section: Discussionmentioning

confidence: 99%

Patient survival by Hsp70 membrane phenotype

Pfister

Radons

Busch

et al. 2007

Cancer

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“…The factors responsible for this distinctive intrahepatic population are uncertain, but could include selective recruitment of those lymphocyte subsets from the periphery and/or local generation and differentiation (12,13). Of particular interest is the fact that NKT cells are far more abundant in the liver than in any other place (10,14,15).…”

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confidence: 99%

“…Unlike in mice, human livers contain few CD1d-restricted NKT cells; instead they are enriched for CD3 ϩ CD56 ϩ NKT cells coexpressing an oligoclonal TCR and NKR such as CD94/NKG2 and killer Ig-like receptor (KIR) 4 (16,17), making even more intriguing the origin of this nonclassical NKT cell population. It has been proposed that the unique hepatic microenvironment, through interactions with either epithelial cells or local cytokines, may shape the development of this distinctive intrahepatic population (11,13,18).…”

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confidence: 99%

Hepatocytes and IL-15: A Favorable Microenvironment for T Cell Survival and CD8+ T Cell Differentiation

Correia

Cardoso

Pereira³

et al. 2009

The Journal of Immunology

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Human intrahepatic lymphocytes are enriched in CD1d-unrestricted T cells coexpressing NKR. Although the origin of this population remains controversial, it is possible to speculate that the hepatic microenvironment, namely epithelial cells or the cytokine milieu, may play a role in its shaping. IL-15 is constitutively expressed in the liver and has a key role in activation and survival of innate and tissue-associated immune cells. In this in vitro study, we examined whether hepatocyte cell lines and/or IL-15 could play a role in the generation of NK-like T cells. The results show that both HepG2 cells and a human immortalized hepatocyte cell line increase survival and drive basal proliferation of T cells. In addition, IL-15 was capable of inducing Ag-independent up-regulation of NKR, including NKG2A, Ig-like receptors, and de novo expression of CD56 and NKp46 in CD8+CD56− T cells. In conclusion, our study suggests that hepatocytes and IL-15 create a favorable microenvironment for T cells to growth and survive. It can be proposed that the increased percentage of intrahepatic nonclassical NKT cells could be in part due to a local CD8+ T cell differentiation.

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“…[7][8][9] This finding may be linked to a decrease in serum interleukin (IL)-15, a key cytokine in the development and maintenance of NK homeostasis, 9 although liver expression of IL-15 may be increased. 19 However, even if one focuses on the CD56 dim population it is not clear that there are clear differences in the cytolytic capabilities of these cells when the number of effector cells is taken into account, as the present study and others demonstrate. 7,14 Part of the reason to define the role of different subsets of NK cells is that it is not clear which function of NKcytolysis or production of cytokines such as IFN␥ -may be more relevant in control of HCV.…”

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confidence: 47%

NK cells: Natural born killers in the conflict between humans and HCV

Koziel

2006

Hepatology

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Hepatic interleuklin 15 (IL-15) expression: implications for local NK/NKT cell homeostasis and development

Cited by 69 publications

References 37 publications

Patient survival by Hsp70 membrane phenotype

Patient survival by Hsp70 membrane phenotype

Hepatocytes and IL-15: A Favorable Microenvironment for T Cell Survival and CD8+ T Cell Differentiation

NK cells: Natural born killers in the conflict between humans and HCV

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