Serum CD163 and TARC as disease response biomarkers in classical Hodgkin lymphoma

K Jones, F Vari, C Keane, P Crooks, JP Nourse… - Clinical cancer …, 2013 - AACR
K Jones, F Vari, C Keane, P Crooks, JP Nourse, LA Seymour, D Gottlieb, D Ritchie, D Gill…
Clinical cancer research, 2013AACR
Purpose: Candidate circulating disease response biomarkers for classical Hodgkin
lymphoma (cHL) might arise from Hodgkin–Reed–Sternberg (HRS) cells or nonmalignant
tumor-infiltrating cells. HRS cells are sparse within the diseased node, whereas benign
CD163+ M2 tissue-associated macrophages (TAM) are prominent. CD163+ cells within the
malignant node may be prognostic, but there is no data on serum CD163 (sCD163). The
HRS-specific serum protein sTARC shows promise as a disease response biomarker …
Abstract
Purpose: Candidate circulating disease response biomarkers for classical Hodgkin lymphoma (cHL) might arise from Hodgkin–Reed–Sternberg (HRS) cells or nonmalignant tumor-infiltrating cells. HRS cells are sparse within the diseased node, whereas benign CD163+ M2 tissue-associated macrophages (TAM) are prominent. CD163+ cells within the malignant node may be prognostic, but there is no data on serum CD163 (sCD163). The HRS-specific serum protein sTARC shows promise as a disease response biomarker. Tumor-specific and tumor-infiltrating circulating biomarkers have not been compared previously.
Experimental Design: We prospectively measured sCD163 and sTARC in 221 samples from 47 patients with Hodgkin lymphoma and 21 healthy participants. Blood was taken at five fixed time-points prior, during, and after first-line therapy. Results were compared with radiological assessment and plasma Epstein-Barr virus DNA (EBV-DNA). Potential sources of circulating CD163 were investigated, along with immunosuppressive properties of CD163.
Results: Pretherapy, both sCD163 and sTARC were markedly elevated compared with healthy and complete remission samples. sCD163 better reflected tumor burden during therapy, whereas sTARC had greater value upon completion of therapy. sCD163 correlated with plasma EBV-DNA, and associated with B symptoms, stage, and lymphopenia. Circulating CD163+ monocytes were elevated in patients, indicating that sCD163 are likely derived from circulating and intratumoral cells. Depletion of cHL CD163+ monocytes markedly enhanced T-cell proliferation, implicating monocytes and/or TAMs as potential novel targets for immunotherapeutic manipulation.
Conclusion: The combination of circulating tumor-infiltrate (sCD163) and tumor-specific (sTARC) proteins is more informative than either marker alone as disease response biomarkers in early and advanced disease during first-line therapy for cHL. Clin Cancer Res; 19(3); 731–42. ©2012 AACR.
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