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Proteomics of REPLICANT perfusate detects changes in the metastatic lymph node microenvironment

Proteomics of REPLICANT perfusate detects changes in the metastatic lymph node microenvironment
AbstractIn breast cancer (BC), detecting low volumes of axillary lymph node (ALN) metastasis pre-operatively is difficult and novel biomarkers are needed. We recently showed that patient-derived ALNs can be sustained ex-vivo using normothermic perfusion. We now compare reactive (tumour-free;n = 5) and macrometastatic (containing tumour deposits >2 mm;n = 4) ALNs by combining whole section multiplex immunofluorescence with TMT-labelled LC-MS/MS of the circulating perfusate. Macrometastases contained significantly fewer B cells and T cells (CD4+/CD8+/regulatory) than reactive nodes (p = 0.02). Similarly, pathway analysis of the perfusate proteome (119/1453 proteins significantly differentially expressed) showed that immune function was diminished in macrometastases in favour of ‘extracellular matrix degradation’; only ‘neutrophil degranulation’ was preserved. Qualitative comparison of the perfusate proteome to that of node-positive pancreatic and prostatic adenocarcinoma also highlighted ‘neutrophil degranulation’ as a contributing factor to nodal metastasis. Thus, metastasis-induced changes in the REPLICANT perfusate proteome are detectable, and could facilitate biomarker discovery.
- The Institute of Cancer Research United Kingdom
- King's College London United Kingdom
- King's College London, University of London
- Imperial College Healthcare NHS Trust United Kingdom
- Institute of Cancer Research United Kingdom
610, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 600, RC254-282, Article
610, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 600, RC254-282, Article
120 Research products, page 1 of 12
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