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Circulating tumor DNA isolated from blood samples in patients with pancreatic adenocarcinoma independently predicted survival, according to prospective study results.
Perspective from
“Circulating tumor DNA (ctDNA) is an attractive biomarker that could help us to define or mange our treatments in the future,” Jean-Baptiste Bachet, MD, PhD, of the gastroenterology and digestive oncology department at Sorbonne University and Centre Universitaire des Saints-Peres in Paris, told HemOnc Today.
To determine whether ctDNA offered prognostic value in pancreatic adenocarcinoma, Bachet and colleagues collected blood samples from 135 patients with resectable (n = 31), locally advanced (n = 36) or metastatic disease (n = 68).
Researchers used next-generation sequencing to target low-allele frequency mutations, and they used picoliter droplet digital polymerase chain reaction to screen samples for several types of mutations, including the three most frequent KRAS mutations in pancreatic adenocarcinoma.
Fifty of the 104 patients (48%) with advanced disease had detectable ctDNA, with a median mutation allelic frequency of 6.1% (range, 0.1-65.4).
Median follow-up for this group was 34.2 months.
Univariate analysis showed a strong correlation between the presence of ctDNA and shorter median OS (6.5 months vs. 19 months; P < .001). Multivariate analysis that accounted for age, sex and disease stage showed an independent association between ctDNA and poor OS (HR = 1.96; 95% CI, 1.2=-3.2).
When researchers analyzed patients with advanced disease based on mutation frequency in ctDNA, they observed a significant dose–response relationship with OS (18.9 months for the lowest tertile, 7.8 months for those in the middle tertile, and 4.9 months for those in the highest tertile; P < .001).
Six of the 31 patients with resectable disease had detectable ctDNA. After median follow-up of 33 months, 23 experienced disease recurrence and 13 had died. Researchers reported longer median DFS (17.6 months vs. 4.6 months) and longer median OS (32.2 months vs. 19.3 months) among patients with no detectable ctDNA.
“Our results are important because they will help future development and assessment of such biomarkers in clinical practice, [including] differences in rate of positive ctDNA according to stage of the disease, grade of differentiation, prognostic value [and] number of mutations found through next-generation sequencing,” Bachet said.
The results should be confirmed in prospective clinical trials to “better assess the predictive value of this biomarker in light of the dynamic biological changes that occur during treatment,” Bachet added. – by Melinda Stevens
Disclosures: Bachet reports advisory board and consultant roles with Amgen, Celgene and Merck Serono.
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