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Computational ranking identifies Plexin-B2 in circulating tumor cell clustering with monocytes in breast cancer metastasis

Nature Communications. 2025-08; 
Emma Schuster, Nurmaa K Dashzeveg, Fangjia Tong, Yuzhi Jia, Lamiaa El-Shennawy, Tong Zhang, Andrew D Hoffman, Reta Birhanu Kitata, Golam Kibria, Youbin Zhang, Joshua R Squires, Chunlei Zheng, Erika Ramos, Rokana Taftaf, David Scholten, Hannah F Almubarak, Valery Adorno-Cruz, David P Sullivan, Carolina Reduzzi, Allegra C Minor, William Purev-Ochir, Sabina Spahija, Rong Xu, Kalliopi P Siziopikou, Leonidas C Platanias, Ami Shah, William A Muller, William J Gradishar, Massimo Cristofanilli, Chia-Feng Tsai, Tujin Shi, Huiping Liu Department of Pharmacology, Northwestern University Feinberg School of Medicine, Chicago, IL, USA.
Products/Services Used Details Operation
Custom Vector Construction pLV-PLXNB2-mRBD (Addgene #86240), pLV-PLXNB2-dVTDL (Addgene 86239), pLV-PLXNB2-dECTO (Addgene #86238), PLXNB2 OHu01778C_pcDNA3.1( + ) N-Terminal Flag-Tag (GenScript #SC1626), PLXNB2 OHu01778D_pcDNA3.1 + /C- C-Terminal Flag-Tag (GeneScript #OHu01778D), PLXNB2 Untagged Construct (GeneScript #SC1625). Get A Quote

Abstract

Multicellular circulating tumor cell (CTC) clusters can be up to 50 times more efficient than single CTCs in mediating viable metastasis. Here, combining computational ranking and functional determination, we identify the transmembrane protein Plexin-B2 (PLXNB2) as one of the top molecular targets associated with unfavorable distant metastasis-free survival, showing enriched expression in CTC clusters versus single CTCs from patients with advanced breast cancer (mostly female). Loss of PLXNB2 (Plxnb2) reduces the formation of homotypic tumor cell clusters and heterotypic tumor-myeloid cell clusters, reducing spontaneous metastases in female mice bearing human (mouse) breast cancer. Interactions of PLXNB2 with i... More

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