Design of a peptidic inhibitor that targets the dimer interface of a prototypic galectin

Vladoiu, Maria C.; Labrie, Marilyne; Létourneau, Myriam; Egesborg, Philippe; Gagné, Donald; Billard, Étienne; Grosset, Andrée Anne; Doucet, Nicolas; Chatenet, David; St‐Pierre, Yves

doi:10.18632/oncotarget.5403

Cited by 21 publications

(26 citation statements)

References 51 publications

(43 reference statements)

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“…These findings are of great importance in the design of gal-7 inhibitors for the treatment of various diseases where gal-7 plays a central role, most notably in cancer [ 6 , 7 , 9 ]. These findings suggest that targeting extracellular gal-7 using either CRD-specific inhibitors [ 14 ] or dimer-disrupting peptides (DIPs) [ 13 ] may be more efficient than expected for targeting intracellular gal-7-mediated interactions. Furthermore, our results showing that extracellular gal-7 induces de novo lgals7 gene activation and our approach using FITC-tagged recombinant gal-7 to follow the fate of extracellular gal-7 inside the cells provide new and original in vitro model systems to investigate the inhibitory activity of these gal-7-specific inhibitors.…”

Section: Discussionmentioning

confidence: 99%

“…Production of human recombinant gal-7 was carried out as described using a pET-22b(+) plasmid encoding a synthetic, codon-optimized cDNA [ 13 ]. In some experiments, recombinant gal-7 was labeled with fluorescein isothiocyanate (FITC) as described [ 13 ]. FITC-labeled gal-7 was purified using a PD-10 Sepharose column (GE healthcare) and eluted with PBS.…”

Section: Methodsmentioning

confidence: 99%

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Intracellular galectin-7 expression in cancer cells results from an autocrine transcriptional mechanism and endocytosis of extracellular galectin-7

Bibens-Laulan

St‐Pierre

2017

PLoS ONE

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The β-galactoside binding protein galectin-7 (gal-7) is constitutively expressed at abnormally high levels in the outside milieu and intracellular compartments of many types of epithelial cancer cells, most notably in aggressive forms of ovarian and breast cancer. It is thus of utmost importance to understand how gal-7 traffics between both intracellular and extracellular compartments to develop novel drugs that target the protumorigenic functions of galectin-7. In the present work, we report that extracellular gal-7 plays a central role in controlling intracellular gal-7 in cells. It does so via two distinct yet complementary mechanisms: firstly by increasing the transcriptional activation of lgals7 gene transcription, and secondly via re-entry into the cells. Increased mRNA levels were dose- and time-dependent and occur in all cell lines tested, including ovarian and breast cancer cell lines. Addition of recombinant gal-7 to MDA-MB-231 transfected with a luciferase reporter vector containing response elements of the lgals7 promoter indicated that increased mRNA level of lgals7 occurs via de novo gene transcription. Re-entry of extracellular gal-7 inside cells was rapid, and reached cytosolic and mitochondrial compartments. Taken together, these findings reveal the existence of a positive self-amplification pathway that regulates intracellular gal-7 expression in breast and ovarian cancer cells.

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Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Intracellular galectin-7 expression in cancer cells results from an autocrine transcriptional mechanism and endocytosis of extracellular galectin-7

Bibens-Laulan

St‐Pierre

2017

PLoS ONE

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“…Serum galectin-7 concentration is a promising prospective biomarker for predicting subsequent miscarriage or the development of preeclampsia in pregnancy (15,23). Galectin-7 may also have potential as a therapeutic target to treat EC, and inhibitors are currently being developed (38) and could be tested in mouse models of EC. Overall, the present study has identified galectin-7 as a novel mediator of EC progression.…”

Section: Discussionmentioning

confidence: 99%

Galectin‑7 is elevated in endometrioid (type I) endometrial cancer and promotes cell migration

et al. 2018

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Endometrial cancer (EC) is the most commonly diagnosed gynecological malignancy in Australian women. Notably, its incidence and mortality rate is increasing. Despite this, there are limited treatment options for EC. Galectin-7 regulates tumorigenesis in numerous epithelial cancer types, but the role of galectin-7 has not been investigated in EC. It was hypothesized that galectin-7 expression would be altered in EC and contribute to the development of EC. Galectin-7 levels in EC and benign endometrium were quantified by reverse transcription-quantitative polymerase chain reaction (RT-qPCR) and ELISA. The effect of recombinant galectin-7 (1 µg/ml) on cell adhesion, proliferation, apoptosis (xCELLigence and flow cytometry), migration (wound healing assay) and gene expression (RT-qPCR) was investigated using three human EC cell lines (Ishikawa, HEC1A and AN3CA). Galectin-7 gene and protein expression was significantly elevated in Grade 3 EC, compared with benign tissues. Galectin-7 was almost undetectable in Ishikawa and AN3CA cells, but highly expressed by HEC1A cells. Recombinant galectin-7 had no significant effect on cell proliferation or apoptosis in any cell line, but significantly reduced cell adhesion in Ishikawa (at 4 and 6 h) and AN3CA (at 2, 3, 4 and 6 h). Galectin-7 significantly promoted Ishikawa migration and significantly elevated collagen type IV α 1 chain and intercellular adhesion molecule 1 (ICAM1) gene expression during wound healing. The present study demonstrated that galectin-7 production increased in EC with increasing cancer grade; therefore, galectin-7 may promote the metastasis of EC by reducing cell-cell adhesion and enhancing cell migration.

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“…Moreover, extracellular Gal7 induced T-cell apoptosis whereas intracellularly this lectin controlled proliferation and differentiation of keratinocytes through mechanisms involving the JNK1, miR-203 and p63 signaling pathways (120)(121)(122). Enforced expression of Gal7 in cancer cells controlled several molecular networks involved in metabolism, survival and immunity (123).…”

Section: H Other Galectinsmentioning

confidence: 99%

Galectins: Key Players at the Frontiers of Innate and Adaptive Immunity

Allo

Toscano

Pinto

et al. 2018

TIGG

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The proper function of the immune system entails multiple regulatory pathways aimed at modulating immunogenic and tolerogenic functions of immune cells. Galectins, a family of carbohydrate-binding proteins, control a variety of biological processes involved in activation, differentiation, trafficking and survival of immune cells. In this review we summarize pioneer work and emerging findings highlighting selected functions of galectins as regulatory checkpoints that control innate and adaptive immune cell programs.

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Design of a peptidic inhibitor that targets the dimer interface of a prototypic galectin

Cited by 21 publications

References 51 publications

Intracellular galectin-7 expression in cancer cells results from an autocrine transcriptional mechanism and endocytosis of extracellular galectin-7

Intracellular galectin-7 expression in cancer cells results from an autocrine transcriptional mechanism and endocytosis of extracellular galectin-7

Galectin‑7 is elevated in endometrioid (type I) endometrial cancer and promotes cell migration

Galectins: Key Players at the Frontiers of Innate and Adaptive Immunity

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