C1q acts in the tumour microenvironment as a cancer-promoting factor independently of complement activation

Bulla, Roberta; Tripodo, Claudio; Rami, Damiano; Ling, Guang Sheng; Agostinis, Chiara; Guarnotta, Carla; Zorzet, Sonia; Durigutto, Paolo; Botto, Marina; Tedesco, Francesco

doi:10.1038/ncomms10346

Cited by 231 publications

(253 citation statements)

References 66 publications

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“…Irrespectively of the beneficial or harmful impact that the complement system has on tumor growth, the C1q molecule's contribution to tumor progression and metastasization has been demonstrated regardless of complement activation, both in prostatic cancer cells 15,35 and very recently in melanoma. 31 These results provide a new perspective on our previously published data which demonstrated that the neuT upregulation on tumor cells observed in neuT-C3KO tumors was not only directly dependent on lack of C3 activation. In particular, the extremely aggressive phenotype displayed by neuT-C3KO tumors can also be caused by the impaired activation of WWOX, which is a result of the unexpected lack of C1q deposition on the tumor site of neuT-C3KO mice.…”

Section: Discussionsupporting

confidence: 69%

“…It has been demonstrated that cancer cells establish a balance between complement activation and inhibition. 29 However, controversial and conflicting data on the complement system's tumor-promoting, 30,31 and inhibiting activities, 24 have been published, 2 and the mechanisms of complement-specific activities in the tumor microenvironment are still unclear and demands further study.…”

Section: Discussionmentioning

confidence: 99%

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The non-inflammatory role of C1q during Her2/neu-driven mammary carcinogenesis

et al. 2016

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There is an ever increasing amount of evidence to support the hypothesis that complement C1q, the first component of the classical complement pathway, is involved in the regulation of cancer growth, in addition to its role in fighting infections. It has been demonstrated that C1q is expressed in the microenvironment of various types of human tumors, including breast adenocarcinomas. This study compares carcinogenesis progression in C1q deficient (neuT-C1KO) and C1q competent neuT mice in order to investigate the role of C1q in mammary carcinogenesis. Significantly accelerated autochthonous neu C carcinoma progression was paralleled by accelerated spontaneous lung metastases occurrence in C1q deficient mice. Surprisingly, this effect was not caused by differences in the tumor-infiltrating cells or in the activation of the complement classical pathway, since neuT-C1KO mice did not display a reduction in C3 fragment deposition at the tumor site. By contrast, a significant higher number of intratumor blood vessels and a decrease in the activation of the tumor suppressor WW domain containing oxidoreductase (WWOX) were observed in tumors from neuT-C1KO as compare with neuT mice. In parallel, an increase in Her2/neu expression was observed on the membrane of tumor cells. Taken together, our findings suggest that C1q plays a direct role both on halting tumor angiogenesis and on inducing apoptosis in mammary cancer cells by coordinating the signal transduction pathways linked to WWOX and, furthermore, highlight the role of C1q in mammary tumor immune surveillance regardless of complement system activation.Abbreviations: BALB-C1KO, BALB/c mice deficient for the C1qA; BALB-C3KO, BALB/c mice deficient for C3; C1KO, C1q deficient; C1qR, C1q receptor; CR3, complement receptor 3; EMT, epithelial-to-mesenchymal transition; KLRK1 or NKG2D, killer cell lectin-like receptor subfamily K, member 1; MDCS, myeloid-derived suppressor cells; neuT, rat Her2/neu transgenic; neuT-BKO mice, neuT mice deficient in antibody production; neuT-C1KO mice, neuT mice deficient for the C1qA molecule; neuT-C3KO mice, neuT mice deficient for the C3 molecule; NK, natural killer; pWWOX, phospho WWOX; Treg, T regulatory; WWOX, WW domain containing oxidoreductase

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Section: Discussionsupporting

confidence: 69%

Section: Discussionmentioning

confidence: 99%

The non-inflammatory role of C1q during Her2/neu-driven mammary carcinogenesis

et al. 2016

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“…Recently, a wide range of immunomodulatory functions of C1q have become evident that are independent of its involvement in the complement activation (3,4); these include modulation of dendritic cell functions (5), cancer progression (6), and neuronal synapse pruning (7).…”

mentioning

confidence: 99%

Human c1q induces apoptosis in an ovarian cancer cell line via tumor necrosis factor pathway

Kaur

Sultan

Murugaiah

et al. 2017

Molecular Immunology

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“…Certaines protéines du complément comme le C1q et les anaphylatoxines C3a et C5a, peuvent participer à ce processus. Ainsi, dans le modèle de mélanome B16/F10 [26], les souris déficientes pour le gène codant le C1q présentent une croissance tumorale ralentie qui peut être reliée, notamment, à une densité du réseau vasculaire des tumeurs diminuée. Cet effet du C1q sur la vascularisation a également été rapporté dans des modèles in vitro utilisant des cellules endothéliales, mais également in vivo, dans le cadre de la pré-éclampsie [36] ou de la cicatrisation des plaies [37].…”

Section: Resultsunclassified

“…De récentes études ont en effet montré que le C1q et le CAM possédaient également des propriétés pro-mitogéniques et prométastatiques. Ainsi, dans le modèle murin syngénique de mélanome B16/F10 2 , la croissance tumorale observée chez des souris déficientes pour le gène codant C1q est ralentie et la survie des animaux est prolongée [26]. Le C1q agit directement sur les cellules tumorales dont il augmente l'adhérence, la migration et la prolifération.…”

Section: Protéines Du Complément Et Contexte Tumoralunclassified