Your search keyword '"Hammadi Mehdi"' showing total 5 results

1. TRPM8 as an Anti–Tumoral Target in Prostate Cancer Growth and Metastasis Dissemination.

Author

Grolez, Guillaume P., Chinigò, Giorgia, Barras, Alexandre, Hammadi, Mehdi, Noyer, Lucile, Kondratska, Kateryna, Bulk, Etmar, Oullier, Thibauld, Marionneau-Lambot, Séverine, Le Mée, Marilyne, Rétif, Stéphanie, Lerondel, Stéphanie, Bongiovanni, Antonino, Genova, Tullio, Roger, Sébastien, Boukherroub, Rabah, Schwab, Albrecht, Fiorio Pla, Alessandra, and Gkika, Dimitra

Subjects

METASTASIS, PROSTATE cancer, TUMOR growth, FOCAL adhesions, CELL proliferation, MEMBRANE lipids

Abstract

In the fight against prostate cancer (PCa), TRPM8 is one of the most promising clinical targets. Indeed, several studies have highlighted that TRPM8 involvement is key in PCa progression because of its impact on cell proliferation, viability, and migration. However, data from the literature are somewhat contradictory regarding the precise role of TRPM8 in prostatic carcinogenesis and are mostly based on in vitro studies. The purpose of this study was to clarify the role played by TRPM8 in PCa progression. We used a prostate orthotopic xenograft mouse model to show that TRPM8 overexpression dramatically limited tumor growth and metastasis dissemination in vivo. Mechanistically, our in vitro data revealed that TRPM8 inhibited tumor growth by affecting the cell proliferation and clonogenic properties of PCa cells. Moreover, TRPM8 impacted metastatic dissemination mainly by impairing cytoskeleton dynamics and focal adhesion formation through the inhibition of the Cdc42, Rac1, ERK, and FAK pathways. Lastly, we proved the in vivo efficiency of a new tool based on lipid nanocapsules containing WS12 in limiting the TRPM8–positive cells' dissemination at metastatic sites. Our work strongly supports the protective role of TRPM8 on PCa progression, providing new insights into the potential application of TRPM8 as a therapeutic target in PCa treatment. [ABSTRACT FROM AUTHOR]

Published

2022

2. Epigenetic dysregulation of KCa3.1 channels induces poor prognosis in lung cancer.

Author

Bulk, Etmar, Ay, Anne‐Sophie, Hammadi, Mehdi, Ouadid‐Ahidouch, Halima, Schelhaas, Sonja, Hascher, Antje, Rohde, Christian, Thoennissen, Nils H., Wiewrodt, Rainer, Schmidt, Eva, Marra, Alessandro, Hillejan, Ludger, Jacobs, Andreas H., Klein, Hans‐Ulrich, Dugas, Martin, Berdel, Wolfgang E., Müller‐Tidow, Carsten, and Schwab, Albrecht

Abstract

Epigenomic changes are an important feature of malignant tumors. How tumor aggressiveness is affected by DNA methylation of specific loci is largely unexplored. In genome-wide DNA methylation analyses, we identified the KCa3.1 channel gene (KCNN4) promoter to be hypomethylated in an aggressive non-small-cell lung carcinoma (NSCLC) cell line and in patient samples. Accordingly, KCa3.1 expression was increased in more aggressive NSCLC cells. Both findings were strong predictors for poor prognosis in lung adenocarcinoma. Increased KCa3.1 expression was associated with aggressive features of NSCLC cells. Proliferation and migration of pro-metastatic NSCLC cells depended on KCa3.1 activity. Mechanistically, elevated KCa3.1 expression hyperpolarized the membrane potential, thereby augmenting the driving force for Ca2+ influx. KCa3.1 blockade strongly reduced the growth of xenografted NSCLC cells in mice as measured by positron emission tomography-computed tomography. Thus, loss of DNA methylation of the KCNN4 promoter and increased KCa3.1 channel expression and function are mechanistically linked to poor survival of NSCLC patients. [ABSTRACT FROM AUTHOR]

Published

2015

3. Modulation of ER stress and apoptosis by endoplasmic reticulum calcium leak via translocon during unfolded protein response: involvement of GRP78.

Author

Hammadi, Mehdi, Oulidi, Agathe, Gackière, Florian, Katsogiannou, Maria, Slomianny, Christian, Roudbaraki, Morad, Dewailly, Etienne, Delcourt, Philippe, Lepage, Gilbert, Lotteau, Sabine, Ducreux, Sylvie, Prevarskaya, Natalia, and Van Coppenolle, Fabien

Subjects

ENDOPLASMIC reticulum, CELL physiology, APOPTOSIS, PHYSIOLOGICAL stress, PUROMYCIN, HOMEOSTASIS

Abstract

The endoplasmic reticulum (ER) is involved in many cellular functions, including protein folding and Ca2+ homeostasis. The ability of cells to respond to the ER stress is critical for cell survival, and disruption in such regulation can lead to apoptosis. ER stress is accompanied by alterations in Ca2+ homeostasis, and the ER Ca2+ store depletion by itself can induce ER stress and apoptosis. Despite that, the ER Ca2+ leak channels activated in response to the ER stress remain poorly characterized. Here we demonstrate that ER Ca2+ depletion during the ER stress occurs via translocon, the ER protein complex involved in translation. Numerous ER stress inducers stimulate the ER Ca2+ leak that can be prevented by translocon inhibitor, anisomycin. Expression of GRP78, an ER stress marker, increased following treatment with puromycin (a translocon opener) and was suppressed by anisomycin, confirming a primary role of translocon in ER stress induction. Inhibition of ER store depletion by anisomycin significantly reduces apoptosis stimulated by the ER stress inducers. We suggest that translocon opening is physiologically modulated by GRP78, particularly during the ER stress. The ability to modulate the ER Ca2+ permeability and subsequent ER stress can lead to development of a novel therapeutic approach. [ABSTRACT FROM AUTHOR]

Published

2013

4. Human ether à-gogo K+ channel 1 (hEag1) regulates MDA-MB-231 breast cancer cell migration through Orai1-dependent calcium entry.

Author

Hammadi, Mehdi, Chopin, Valérie, Matifat, Fabrice, Dhennin-Duthille, Isabelle, Chasseraud, Maud, Sevestre, Henri, and Ouadid-Ahidouch, Halima

Subjects

BREAST cancer, CANCER cells, CELL proliferation, DUCTAL carcinoma, CELL migration, CALCIUM channels

Abstract

Breast cancer (BC) has a poor prognosis due to its strong metastatic ability. Accumulating data present ether à go-go (hEag1) K+ channels as relevant player in controlling cell cycle and proliferation of non-invasive BC cells. However, the role of hEag1 in invasive BC cells migration is still unknown. In this study, we studied both the functional expression and the involvement in cell migration of hEag1 in the highly metastatic MDA-MB-231 human BC cells. We showed that hEag1 mRNA and proteins were expressed in human invasive ductal carcinoma tissues and BC cell lines. Functional activity of hEag1 channels in MDA-MB-231 cells was confirmed using astemizole, a hEag1 blocker, or siRNA. Blocking or silencing hEag1 depolarized the membrane potential and reduced both Ca2+ entry and MDA-MB-231 cell migration without affecting cell proliferation. Recent studies have reported that Ca2+ entry through Orai1 channels is required for MDA-MB-231 cell migration. Down-regulation of hEag1 or Orai1 reduced Ca2+ influx and cell migration with similar efficiency. Interestingly, no additive effects on Ca2+ influx or cell migration were observed in cells co-transfected with sihEag1 and siOrai1. Finally, both Orai1 and hEag1 are expressed in invasive breast adenocarcinoma tissues and invaded metastatic lymph node samples (LNM+). In conclusion, this study is the first to demonstrate that hEag1 channels are involved in the serum-induced migration of BC cells by controlling the Ca2+ entry through Orai1 channels. hEag1 may therefore represent a potential target for the suppression of BC cell migration, and thus prevention of metastasis development. J. Cell. Physiol. 227: 3837-3846, 2012. © 2012 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2012

5. TRPM8-androgen receptor association within lipid rafts promotes prostate cancer cell migration.

Author

Grolez, Guillaume P., Gordiendko, Dmitri V., Clarisse, Manon, Hammadi, Mehdi, Desruelles, Emilie, Fromont, Gaëlle, Prevarskaya, Natalia, Slomianny, Christian, and Gkika, Dimitra

Published

2019