Clinical significance of the induction of macrophage differentiation by the costimulatory molecule B7-H3 in human non-small cell lung cancer

Sun, Jing; Mao, Yong; Zhang, Yang‐Qin; Guo, Yundi; Mu, Chuanyong; Fu, Fengqing; Zhang, Xueguang

doi:10.3892/ol.2013.1586

Cited by 29 publications

(24 citation statements)

References 38 publications

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“…We first established that B7-H3 is expressed in NSCLC cells and correlates with a reduction in the number of TILs in tumour tissues [28]. Other groups have demonstrated that B7-H3 expression clearly inhibits T cell-mediated antitumour immunity in NSCLC [15,16]. Interestingly, we also previously demonstrated that ILT4 expression in NSCLC cells is negatively correlated with the number of TILs, indicating a potential role of ILT4 in the inhibition of T cell function in the tumour environment similar to that of B7-H3 [10].…”

Section: Discussionmentioning

confidence: 98%

ILT4 drives B7‐H3 expression via PI3K/AKT/mTOR signalling and ILT4/B7‐H3 co‐expression correlates with poor prognosis in non‐small cell lung cancer

Zhang

et al. 2015

FEBS Letters

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Edited by W. EllmeierKeywords: ILT4 B7-H3 PI3K/AKT/mTOR signalling Non-small cell lung cancer a b s t r a c t Immunoglobulin-like transcript (ILT) 4 is critical for the inhibitory function of certain immune cells. We previously demonstrated that ILT4 is over-expressed in human non-small cell lung cancer (NSCLC) cells and is involved in tumour evasion via an unknown mechanism. In this report, we demonstrate that ILT4 increases the expression of the co-inhibitory molecule B7-H3 through PI3K/AKT/mTOR signalling. In primary human NSCLC tissues, a significant positive relationship is observed between ILT4 and B7-H3 expression. ILT4/B7-H3 co-expression is significantly associated with a reduction in T infiltrating lymphoid cells and lower overall survival. In summary, ILT4 increases B7-H3 expression and ILT4/B7-H3 co-expression may be involved in NSCLC progression.

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Section: Discussionmentioning

confidence: 98%

ILT4 drives B7‐H3 expression via PI3K/AKT/mTOR signalling and ILT4/B7‐H3 co‐expression correlates with poor prognosis in non‐small cell lung cancer

Zhang

et al. 2015

FEBS Letters

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“…Zhang et al found that circulating B7-H3 in serum is a highly sensitive biomarker for non-small cell lung cancer (NSCLC), and increased circulating B7-H3 suggests a poor clinical prognosis for NSCLC (28). Sun et al reported that in the NSCLC environment the B7-H3 signaling pathway may be involved in switching macrophages to the M2 phenotype and the negative regula tion of the T lymphocyte-mediated immune response, thus they hypothesized that B7-H3 is important in NSCLC progression (29). Qin et al found that the specific expression of B7-H3 in tumors and tumor vasculature in clear cell renal cell carcinoma makes it a useful target and prominent biomarker for tumor-specific antiangiogenic therapies.…”

Section: Discussionmentioning

confidence: 99%

Aberrant expression of B7-H3 in gastric adenocarcinoma promotes cancer cell metastasis

et al. 2014

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B7-H3 belongs to the B7 superfamily, a group of molecules that costimulate or downmodulate T cell responses. Although it has been shown that B7-H3 can inhibit T cell responses, several studies, most of them performed in murine systems, found B7-H3 to act in a co-stimulatory manner. In addition, B7-H3 is also expressed in various human cancers and is correlated with the poor outcome of cancer patients. The functional role of B7-H3 in cancer is still controversially discussed. In the present study, we compared B7-H3 expression in normal gastric tissues and gastric cancer tissue specimens and determined the effects of low B7-H3 expression on the human gastric cancer cell line SGC-7901 by using RNAi. B7-H3 expression in gastric specimens was determined by tissue qPCR and immunohistochemisty. A SGC-7901 cell line with low B7-H3 expression was established by lentiviral-mediated RNA interference to investigate the effect of B7-H3 on cancer cell migration and invasion in vitro. By establishing an orthotopic transplantation gastric cancer mouse model, the effect of B7-H3 on cell migration and invasion was studied in vivo. B7-H3 expression was significantly higher in the gastric cancer group than that in the normal gaster group. B7-H3 knockdown by RNA interference decreased cell migration and Transwell invasion up to 50% in vitro. In the orthotopic transplantation gastric cancer mouse model, the effect of inhibiting metastasis by knockdown of B7-H3 was assessed in terms of the average postmortem abdominal visceral metastatic tumor weight. The results revealed that inhibition of B7-H3 expression reduced gastric cancer metastasis in vivo. In conclusion, B7-H3 is aberrantly expressed in gastric cancer. In addition to modulating tumor immunity, B7-H3 may have a novel role in regulating SGC-7901 cell metastasis.

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“…Recently, numerous studies have revealed that B7-H3 is abnormally up-regulated in a variety of cancers, whereas the B7-H4 protein is barely detected in the majority of normal human tissues [24,25]. In addition, overexpression of B7-H3 has been suggested to be positively correlated with tumor size, progression and prognosis [25].…”

Section: Discussionmentioning

confidence: 99%

Astragaloside IV Enhances Cisplatin Chemosensitivity in Non-Small Cell Lung Cancer Cells Through Inhibition of B7-H3

Liu

et al. 2016

Cell Physiol Biochem

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Background: Chemoresistance is a major obstacle to successful chemotherapy for human non-small cell lung cancer (NSCLC). Astragaloside IV, the component of Astragalus membranaceus, has been reported to exhibit anti-inflammation, anti-cancer and immunoregulatory properties. In the present study, we investigated the role of astragaloside IV in the chemoresistance to cisplatin in NSCLC cells. Methods: We established astragaloside IV-suppressed NSCLC cell lines including A549, HCC827, and NCI-H1299 and evaluated their sensitivity to cisplatin in vitro. In addition, we examined the mRNA and protein levels of B7-H3 in response to cisplatin-based chemotherapy. Results: We showed that high doses of astragaloside IV (10, 20, 40 ng/ml) inhibited NSCLC cell growth, whereas low concentrations of astragaloside IV (1, 2.5, 5 ng/ml) had no obvious cytotoxicity on cell viability. Moreover, combined treatment with astragaloside IV significantly increased chemosensitivity to cisplatin in NSCLC cells. On the molecular level, astragaloside IV co-treatment significantly inhibited the mRNA and protein levels of B7-H3 in the presence of cisplatin. In addition, ectopic expression of B7-H3 diminished the sensitization role of astragaloside IV in cellular responses to cisplatin in NSCLC cells. Conclusion: These results demonstrate that astragaloside IV enhances chemosensitivity to cisplatin via inhibition of B7-H3 and that treatment with astragaloside IV and inhibition of B7-H3 serve as potential therapeutic approach for lung cancer patients.

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Clinical significance of the induction of macrophage differentiation by the costimulatory molecule B7-H3 in human non-small cell lung cancer

Cited by 29 publications

References 38 publications

ILT4 drives B7‐H3 expression via PI3K/AKT/mTOR signalling and ILT4/B7‐H3 co‐expression correlates with poor prognosis in non‐small cell lung cancer

ILT4 drives B7‐H3 expression via PI3K/AKT/mTOR signalling and ILT4/B7‐H3 co‐expression correlates with poor prognosis in non‐small cell lung cancer

Aberrant expression of B7-H3 in gastric adenocarcinoma promotes cancer cell metastasis

Astragaloside IV Enhances Cisplatin Chemosensitivity in Non-Small Cell Lung Cancer Cells Through Inhibition of B7-H3

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