Biomarkers of systemic inflammation provide additional prognostic stratification in cancers of unknown primary

Author:

Harvey Svenja1,Stares Mark12ORCID,Scott Julie‐Anne3,Thottiyil Tharun Joseph Vattam4,Conway Alicia‐Marie56,Haigh Rachel2,Brown Jackie2,Knowles Gillian2,Dasgupta Sonali7,Shiu Kai‐Keen4,Mitchell Claire6,Barrie Colin2,Cook Natalie3,Clive Sally2

Affiliation:

1. University of Edinburgh, Cancer Research UK Edinburgh Centre, Institute of Genetics and Cancer, Western General Hospital Edinburgh UK

2. Edinburgh Cancer Centre, NHS Lothian Western General Hospital Edinburgh UK

3. Experimental Cancer Medicine Team (ECMT) The Christie NHS Foundation Trust Manchester UK

4. University College London Hospitals NHS Foundation Trust London UK

5. The University of Manchester, Cancer Research UK Manchester Institute Manchester UK

6. The Christie NHS Foundation Trust Manchester UK

7. Velindre University NHS Trust Cardiff UK

Abstract

AbstractBackgroundBiomarkers of systemic inflammation have been shown to predict outcomes in patients with cancer of unknown primary (CUP). We sought to validate these findings in patients with confirmed CUP (cCUP) and explore their role alongside existing clinicopathological prognostic categories.Patients and MethodsCUP oncologist from across the United Kingdom were invited to include patients with cCUP referred to their local CUP multidisciplinary team. Patient demographics, clinical, pathological and outcome data were recorded and analysed.ResultsData were available for 548 patients from four CUP services. 23% (n = 124) of patients met clinicopathological criteria for favourable‐risk cCUP. On multivariate analysis c‐reactive protein (CRP) (p < 0.001) and the Scottish Inflammatory Prognostic Score (SIPS: combining albumin and neutrophil count) (p < 0.001) were independently predictive of survival. CRP and SIPS effectively stratified survival in patients with both favourable‐risk and poor‐risk cCUP based on clinicopathological features.ConclusionsBiomarkers of systemic inflammation are reliable prognostic factors in patients with cCUP, regardless of clinicopathological subgroup. We recommend that CRP or SIPS are incorporated into routine clinical assessments of patients with cCUP as a tool to aid investigation and/or treatment decision‐making across all groups. Established clinicopathological factors can then be used to inform management pathways and specific systemic anticancer therapy selection.

Publisher

Wiley

Reference40 articles.

1. NICE clinical guideline.National Institute for Health and Clinical Excellence. 2010. Metastatic malignant disease of unknown primary origin [Internet]. Available from:https://www.nice.org.uk/search?q = Metastatic+malignant+disease+of+unknown+primary+origin

2. Cancers of unknown primary site: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up

3. Characterisation and outcomes of patients referred to a regional cancer of unknown primary team: a 10-year analysis

4. CRUK.Cancer Research UK Cancer of Unknown Primary Statistics [Internet].2020Available from:https://www.cancerresearchuk.org/health‐professional/cancer‐statistics/statistics‐by‐cancer‐type/cancer‐of‐unknown‐primary#heading‐Zero

5. Cancer of unknown primary: ESMO clinical practice guideline for diagnosis, treatment and follow‐up. Ann Oncol off J Eur Soc;Krämer A;Med. Oncol.,2023

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