Impaired involution of mammary glands in the absence of milk fat globule EGF factor 8

Hanayama, Rikinari; Nagata, Shinji

doi:10.1073/pnas.0508599102

Cited by 120 publications

(125 citation statements)

References 36 publications

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“…Of note, plasminogen-deficient mice display delayed involution of the mammary glands (24,25). This process is closely linked to apoptotic cell removal and comparably impaired in mice lacking the engulfment factor MFG-E8 (26). Further studies will help to elucidate whether plasminogen deficiency is associated with defects in corpse clearance and the onset of chronic inflammation and autoimmunity.…”

Section: Discussionmentioning

confidence: 99%

Serum-Derived Plasminogen Is Activated by Apoptotic Cells and Promotes Their Phagocytic Clearance

Rosenwald

Koppe

Keppeler

et al. 2012

The Journal of Immunology

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The elimination of apoptotic cells, called efferocytosis, is fundamentally important for tissue homeostasis and prevents the onset of inflammation and autoimmunity. Serum proteins are known to assist in this complex process. In the current study, we performed a multistep chromatographic fractionation of human serum and identified plasminogen, a protein involved in fibrinolysis, wound healing, and tissue remodeling, as a novel serum-derived factor promoting apoptotic cell removal. Even at levels significantly lower than its serum concentration, purified plasminogen strongly enhanced apoptotic prey cell internalization by macrophages. Plasminogen acted mainly on prey cells, whereas on macrophages no enhancement of the engulfment process was observed. We further demonstrate that the efferocytosis-promoting activity essentially required the proteolytic activation of plasminogen and was completely abrogated by the urokinase plasminogen activator inhibitor-1 and serine protease inhibitor aprotinin. Thus, our study assigns a new function to plasminogen and plasmin in apoptotic cell clearance.

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Section: Discussionmentioning

confidence: 99%

Serum-Derived Plasminogen Is Activated by Apoptotic Cells and Promotes Their Phagocytic Clearance

Rosenwald

Koppe

Keppeler

et al. 2012

The Journal of Immunology

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“…In line with this, functionally blocking antibodies against MFG-E8 potentiated the effects of chemotherapeutic agents on experimental melanomas, colon carcinomas and lymphomas (Jinushi et al, 2009). In the mammary gland, MFG-E8 expression increases during pregnancy, lactation and subsequent mammary gland involution (Oshima et al, 1999;Hanayama and Nagata, 2005). It was demonstrated that MFG-E8 is required for mammary gland branching morphogenesis (Ensslin and Shur, 2007).…”

Section: Introductionmentioning

confidence: 93%

“…The binding of MFG-E8 to integrins on macrophages and to phosphatidylserine and phosphatidylethanolamine residues on apoptotic cells establishes intercellular interactions that promote the subsequent engulfment of apoptotic cells (Hanayama et al, 2002(Hanayama et al, , 2004. Similarly, MFG-E8 is required for the removal of apoptotic cells by mammary epithelial cells during mammary gland involution (Atabai et al, 2005;Hanayama and Nagata, 2005). MFG-E8 binding to integrins regulates a variety of signaling pathways.…”

Section: Introductionmentioning

confidence: 99%

MFG-E8/lactadherin regulates cyclins D1/D3 expression and enhances the tumorigenic potential of mammary epithelial cells

et al. 2011

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Milk fat globule-EGF factor 8 (MFG-E8) is a glycoprotein highly expressed in breast cancer that contributes to tumor progression through largely undefined mechanisms. By analyzing publicly available gene expression profiles of breast carcinomas, we found that MFG-E8 is highly expressed in primary and metastatic breast carcinomas, associated with absent estrogen receptor expression. Immunohistochemistry analysis of breast cancer biopsies revealed that MFG-E8 is expressed on the cell membrane as well as in the cytoplasm and nucleus. We also show that increased expression of MFG-E8 in mammary carcinoma cells increases their tumorigenicity in immunodeficient mice, and conversely, its downregulation reduces their in vivo growth. Moreover, expression of MFG-E8 in immortalized mammary epithelial cells promotes their growth and branching in three-dimensional collagen matrices and induces the expression of cyclins D1/D3 and N-cadherin. A mutant protein unable to bind integrins can in part exert these effects, indicating that MFG-E8 function is only partially dependent on integrin activation. We conclude that MFG-E8-dependent signaling stimulates cell proliferation and the acquisition of mesenchymal properties and contributes to mammary carcinoma development.

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“…In contrast, this study dealt with the functional p63 proteins localized to undifferentiated keratinocytes in the basal layer of stratified epithelia and in carcinomas derived from the stage. MFG-E8-L, the mouse-specific long isoform, having a Pro/Thr-enriched domain, facilitates phagocytosis of apoptotic cells by macrophages as demonstrated by recent studies with MFGE8-deficient mice (Hanayama et al, 2002;Hanayama and Nagata, 2005). However, the other isoform, MFG-E8-S, lacking the phagocytosisfacilitating activity is more ubiquitously, abundantly expressed (Watanabe et al, 2005) and expected to facilitate various types of cell-cell interactions.…”

Section: Mfge8mentioning

confidence: 99%

p63(TP63) elicits strong trans-activation of the MFG-E8/lactadherin/BA46 gene through interactions between the TA and ΔN isoforms

et al. 2007

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We report here that human MFGE8 encoding milk fat globule-EGF factor 8 protein (MFG-E8), also termed 46 kDa breast epithelial antigen and lactadherin, is transcriptionally activated by p63, or TP63, a p53 (TP53) family protein frequently overexpressed in head-and-neck squamous cell carcinomas, mammary carcinomas and so on. Despite that human MFG-E8 was originally identified as a breast cancer marker, and has recently been reported to provide peptides for cancer immunotherapy, its transcriptional control remains an open question. Observations in immunohistochemical analyses, a tetracycline-induced p63 expression system and keratinocyte cultures suggested a physiological link between p63 and MFGE8. By reporter assays with immediately upstream regions of MFGE8, we determined that the trans-activator (TA) isoforms of p63 activate MFGE8 transcription though a p53/p63 motif at À370, which was confirmed by a chromatin immunoprecipitation experiment. Upon siRNAmediated p63 silencing in a squamous cell carinoma line, MFG-E8 production decreased to diminish Saos-2 cell adhesion. Interestingly, the DN-p63 isoform lacking the TA domain enhanced the MFGE8-activating function of TA-p63, if DN-p63 was dominant over TA-p63 as typically observed in undifferentiated keratinocytes and squamous cell carcinomas, implying a self-regulatory mechanism of p63 by the TA:DN association. MFG-E8 may provide a novel pathway of epithelial-nonepithelial cell interactions inducible by p63, probably in pathological processes.

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Impaired involution of mammary glands in the absence of milk fat globule EGF factor 8

Cited by 120 publications

References 36 publications

Serum-Derived Plasminogen Is Activated by Apoptotic Cells and Promotes Their Phagocytic Clearance

Serum-Derived Plasminogen Is Activated by Apoptotic Cells and Promotes Their Phagocytic Clearance

MFG-E8/lactadherin regulates cyclins D1/D3 expression and enhances the tumorigenic potential of mammary epithelial cells

p63(TP63) elicits strong trans-activation of the MFG-E8/lactadherin/BA46 gene through interactions between the TA and ΔN isoforms

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