Toll-like receptor expression in normal ovary and ovarian tumors

Zhou, Mingfu; McFarland-Mancini, Molly M.; Funk, Holly M.; Husseinzadeh, Nader; Mounajjed, Taofic; Drew, Angela F.

doi:10.1007/s00262-008-0650-y

Cited by 143 publications

(112 citation statements)

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“…These cancerous TLRs are believed to promote both tumor growth and immune evasion through upregulation of NFκB and production of anti-apoptotic molecules [29,60,61]. A variety of cancer cells and cancer cell lines have been shown to express functionally active TLRs, such as TLR-2, -3, -4, and -5 in ovarian cancer [29,61,62], TLR-3, -4, -5, and -9 in cervical cancer [61,[63][64][65], TLR-9 in lung cancer [43], TLR-4, -5, -9 in gastric cancer [66], and TLR-2, -3, and -4 in colorectal cancer cells lines [67]. In general, TLR-4 and TLR-9 was found to be most strongly expressed in human cancer cells [32].…”

Section: Effects Of Rp215 Anti-human Immunoglobulin G and Anti-t Cementioning

confidence: 99%

Roles of antigen receptors and CA215 in the innate immunity of cancer cells

Lee¹,

Liu²

2013

OJI

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Antigen receptors, including immunoglobulins and T-cell receptors, are known to be widely expressed by cancer cells through unconfirmed mechanisms and for unknown purposes. Recently, a monoclonal antibody, designated as RP215, was generated against the ovarian cancer cell line, OC-3-VGH, and was shown to react with CA215, which consisted mainly of these cancer cell-expressed antigen receptors. Experimental evidence has clearly indicated that cancerous immunoglobulins play significant roles in the growth and proliferation of cancer cells in vitro and in vivo. RP215 and anti-antigen receptor antibodies were equally effective in inducing apoptosis and complement-dependent cytotoxicity reactions to cultured cancer cells. Through gene regulation studies, both RP215 and antibodies against antigen-receptors were shown to affect more than a dozen of genes involved in cell proliferation (such as NFκB-1, IgG, P21, cyclin D1, ribosomal P 1 , and c-fos). Furthermore, selected toll-like receptor genes (TLR-2, -3, -4, and -9) were also found to be highly regulated by both RP215 and anti-antigen receptor antibodies. For example, RP215 and antiantigen receptor antibodies were found to both up-regulate TLR-2 and/or TLR-3 and downregulate TLR-4 and TLR-9 in two types of cancer cells. Based on these studies, it is reasonable to postulate that cancerous immunoglobulins play important roles in the modulation of the innate immune system to allow the growth and survival of cancer cells within the human body. Consequently, RP215 in its humanized forms may be utilized to target cancer cells for potential therapeutic purposes.

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Section: Effects Of Rp215 Anti-human Immunoglobulin G and Anti-t Cementioning

confidence: 99%

Roles of antigen receptors and CA215 in the innate immunity of cancer cells

Lee¹,

Liu²

2013

OJI

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“…Embryonic fibroblasts, 38 cell lines 155 and cancer cells were also known to display various types of TLR. 156 It is important to study how different vital circumstances affect expression of TLRs in cell types and tissues, as well as examination of the difference between in vivo and in vitro.…”

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confidence: 99%

Toll-like Receptor

Takagi

2011

J Clin Exp Hematopathol

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Toll like receptor (TLR), one of the key functions of innate immune system, can recognize not only exogenous pathogenassociated molecular patterns, namely PAMPs, but also endogenous molecules created upon tissue injury, sterile inflammation and degeneration. Endogenous TLR ligands are called as damage-associated molecular patters (DAMPs), including endogenous molecules released by activated and necrotic cells, and extracellular matrix molecules. DAMPs are also known as alarmins. TLR research has brought about new insights in the rheumatic diseases. Previous reports suggest that TLRs and the signal pathways intensively contribute to the pathogenesis of rheumatoid arthritis (RA) and other arthritic conditions with interaction of various TLR ligands. Accumulated knowledge of TLR system is summarized to overlook TLRs and the signaling pathway in arthritis conditions, with special reference to RA. 〔J Clin Exp Hematopathol 51(2) : 77-92, 2011〕

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“…As previously described, chronic TLR activation and signaling in both immune and nonimmune cells by environmental antigens are now linked to oncogenesis, tumor growth, and invasive spread (Schmausser et al, 2005;Kelly et al, 2006;Fukata et al, 2007;He et al, 2007;Ilvesaro et al, 2007;Goto et al, 2008;Kim et al, 2008;Yoneda et al, 2008;Curtin et al, 2009;Xie et al, 2009;Zhou et al, 2009). Activation of TLR signaling results in the activation of transcription factors NF-ĸB and AP-1, as well as Type I Interferon (IFN) signaling pathways with subsequent production of "oncogenic" cytokines, and the activation of MAPK and AKT signaling pathways (Figure 1 prostate and many others ).…”

Section: Mechanisms Of Tlr Regulation Of Carcinogenesismentioning

confidence: 91%