EphA3 targeting reduces in vitro adhesion and invasion and in vivo growth and angiogenesis of multiple myeloma cells

被引:16
作者
La Rocca, Francesco [1 ]
Airoldi, Irma [2 ]
Di Carlo, Emma [3 ,4 ]
Marotta, Pina [5 ]
Falco, Geppino [5 ,6 ]
Simeon, Vittorio [1 ]
Laurenzana, Ilaria [1 ]
Trino, Stefania [1 ]
De Luca, Luciana [1 ]
Todoerti, Katia [1 ]
Villani, Oreste [7 ]
Lackmann, Martin [8 ]
D'Auria, Fiorella [9 ]
Frassoni, Francesco [10 ]
Neri, Antonino [11 ,12 ]
Del Vecchio, Luigi [13 ,14 ]
Musto, Pellegrino [15 ]
Cilloni, Daniela [16 ]
Caivano, Antonella [1 ]
机构
[1] Referral Canc Ctr Basilicata CROB, Lab Preclin & Translat Res, IRCCS, Via Padre Pio 1, I-85028 Rionero In Vulture, Italy
[2] IRCCS G Gaslini Inst, Lab Oncol, Genoa, Italy
[3] BG DAnnunzio Univ, Pathol Anat & Immunooncol Unit, Aging Res Ctr, CeSI MeT, Chieti, Italy
[4] BG DAnnunzio Univ, Dept Med & Sci Aging, Chieti, Italy
[5] Ist Ric Genet Gaetano Salvatore Biogem Scarl, Dept Stem Cell & Dev, Ariano Irpino, Italy
[6] Univ Naples Federico II, Dept Biol, Naples, Italy
[7] IRCCS CROB, Dept Oncohematol, Rionero In Vulture, Italy
[8] Monash Univ, Dept Biochem & Mol Biol, Melbourne, Vic, Australia
[9] IRCCS CROB, Lab Clin Res & Adv Diagnost, Rionero In Vulture, Italy
[10] IRCCS G Gaslini Inst, Lab Cellule Staminali Postnatali & Terapie Cellul, Genoa, Italy
[11] Univ Milan, Dept Clin Sci & Community Hlth, Milan, Italy
[12] Osped Maggiore Policlin, Fdn Ca Granda, Hematol, Milan, Italy
[13] Univ Naples Federico II, Dept Mol Med & Med Biotechnol, Naples, Italy
[14] CEINGE Biotecnol Avanzate Scarl, Naples, Italy
[15] IRCCS CROB, Sci Direct, Rionero In Vulture, Italy
[16] Univ Turin, Dept Clin & Biol Sci, Orbassano, Italy
关键词
Multiple myeloma; Plasma cells; EphA3; Cell movement; Anti EphA3 monoclonal antibody; RECEPTOR TYROSINE KINASE; MOLECULAR CLASSIFICATION; HEMATOLOGIC MALIGNANCIES; THERAPEUTIC TARGET; DRUG-RESISTANCE; EXPRESSION; ANTIBODY; CANCER; LEUKEMIA; HEK;
D O I
10.1007/s13402-017-0338-4
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Multiple myeloma (MM) is a hematologic malignancy characterized by a clonal expansion of plasma cells (PCs) in the bone marrow (BM). Since MM has so far remained incurable, further insights into its pathogenesis and the concomitant identification of new therapeutic targets are urgently needed. The tyrosine kinase receptor EphA3 is known to be involved in various cellular processes including cell viability, cell movement and cell-cell interactions. Recently, EphA3 has emerged as a potential therapeutic target in several hematologic and solid tumors. Here, we aimed to uncover the role of EphA3 in MM. EphA3 mRNA and protein expression in primary MM bone marrow plasma cells (BMPCs), in MM-derived cell lines and in healthy controls (HCs) was assessed using qRT-PCR, Western blotting and flow cytometry. The effects of siRNA-mediated EphA3 silencing and anti EphA3 antibody (EphA3mAb) treatment on MM PC trafficking and viability were evaluated using in vitro assays. The effects of EphA3mAb treatment were also assessed in two MM-derived mouse xenograft models. We found that EphA3 was overexpressed in primary MM BMPCs and MM-derived cell lines compared to HCs. We also found that siRNA-mediated EphA3 silencing and EphA3mAb treatment significantly inhibited the ability of MM PCs to adhere to fibronectin and stromal cells and to invade in vitro, without affecting cell proliferation and viability. Gene expression profiling showed that EphA3 silencing resulted in expression modulation of several molecules that regulate adhesion, migration and invasion processes. Importantly, we found that EphA3mAb treatment significantly inhibited in vivo tumor growth and angiogenesis in two MM-derived mouse xenograft models. Our findings suggest that EphA3 plays an important role in the pathogenesis of MM and provide support for the notion that its targeting may represent a novel therapeutic opportunity for MM.
引用
收藏
页码:483 / 496
页数:14
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