Developing an objective marker to optimize patient selection and predict survival benefit in early-phase cancer trials

Chara Stavraka, David J. Pinato, Samantha J. Turnbull, Michael J. Flynn, Martin D. Forster, Sean M. O'Cathail, Sayed Babar, Michael J. Seckl, Rebecca S. Kristeleit, Sarah P. Blagden

Risultato della ricerca: Contributo su rivistaArticolo in rivistapeer review

Abstract

BACKGROUND Several prognostic indices have been devised to optimize patient selection for phase 1 oncology trials with no consensus as to the optimal score and none qualifying as a marker of treatment response. METHODS Multivariate predictors of overall survival (OS) were tested on 118 referred patients to develop the Hammersmith Score (HS). The score's ability to predict OS, progression-free survival (PFS), and 90-day mortality (90DM) was compared with other prognostic indices. Changes in HS were recalculated during treatment. RESULTS Albumin < 35 g/L, lactate dehydrogenase > 450 U/L, and sodium < 135 mmol/L emerged as independent prognostic factors. These were used with equal weighting to devise the HS, a compound prognostic index ranging from 0 to 3. High (HS = 2-3) score predicted worse OS (hazard ratio [HR] = 6.5, P <.001), PFS (HR = 2.8, P =.01), and 90DM (OR = 9.0, P <.001). HS was a more accurate multivariate predictor of OS (HR = 6.4, P <.001, C-index = 0.72), PFS (HR = 2.7, P =.03), and 90DM (area under the ROC curve 0.703) compared with other scores. Worsening of the HS during treatment predicted for shorter OS (P <.001). HS retained prognostic and predictive ability following external validation. CONCLUSIONS HS is a simple, validated index to optimize patient selection and predict survival benefit from phase 1 oncology treatments. Prospective validation is ongoing.

Lingua originaleInglese
pagine (da-a)262-270
Numero di pagine9
RivistaCancer
Volume120
Numero di pubblicazione2
DOI
Stato di pubblicazionePubblicato - 15 gen 2014
Pubblicato esternamente

Fingerprint

Entra nei temi di ricerca di 'Developing an objective marker to optimize patient selection and predict survival benefit in early-phase cancer trials'. Insieme formano una fingerprint unica.

Cita questo