Longitudinal Glioma Monitoring via Cerebrospinal Fluid Cell-Free DNA

Cecile Riviere-Cazaux,Xiaoxi Dong,Wei Mo,Rahul Kumar,Chao Dai,Lucas P Carlstrom,Amanda Munoz-Casabella,Keyvan Ghadimi,Cody L Nesvick,Katherine M Andersen,Matthew D Hoplin,Nicholas Canaday,Ignacio Jusue-Torres,Noor Malik,Jian L Campian,Michael W Ruff,Joon H Uhm,Jeanette E Eckel Passow,Timothy J Kaufmann,David M Routman,Sani H Kizilbash,Ugur Sener,Arthur E Warrington,Robert B Jenkins,Pan Du,Shidong Jia,Terry C Burns

doi:10.1158/1078-0432.ccr-24-1814

Cecile Riviere-Cazaux, Xiaoxi Dong + Show 25 more

https://doi.org/10.1158/1078-0432.ccr-24-1814

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Journal: Clinical Cancer Research	Publication Date: Jan 30, 2025
License type: CC BY-NC-ND 4.0

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Abstract Purpose: Current methods for glioma response assessment are limited. This study aimed to assess the technical and clinical feasibility of molecular profiling using longitudinal intracranial cerebrospinal fluid (CSF) from patients with gliomas. Experimental Design: Adults with gliomas underwent longitudinal intracranial CSF collection via Ommaya reservoirs or ventriculoperitoneal shunts. Cell-free DNA (cfDNA) was extracted and analyzed using PredicineCARE for cancer variant profiling and/or PredicineSCORE for low-pass whole-genome sequencing. Results: Five patients (two females and three males; median age, 40 years; range, 32–64 years) underwent longitudinal intracranial CSF collection via Ommaya reservoirs (n = 4) or ventriculoperitoneal shunts (n = 1). In total, 47 CSF samples were obtained (median volume, 4.00 mL; 0.5–5 mL). Forty-one samples (87.2%) yielded sufficient cfDNA for testing. Patient-specific tumor-associated variant allelic frequencies (VAF), and thus tumor fraction, decreased in pre- versus postchemoradiation samples, including through pseudoprogression. These also increased with radiographic progression in three patients, although identifying the time of definitive disease progression from MRIs was a significant limitation. In two patients with isocitrate dehydrogenase (IDH)–mutant gliomas, decreasing IDH1 VAF after resection and chemoradiation correlated with decreased CSF D-2-hydroxyglutarate levels (0.64× and 0.62×, respectively, for the first patient and 0.01× and 0.07× for the other patient), although D-2-hydroxyglutarate and IDH1 VAF were not concordant in one patient thereafter. Moreover, the copy-number burden decreased below the limit of quantification during treatment and increased above the limit at progression. Conclusions: Longitudinal intracranial CSF cfDNA can be obtained in patients with gliomas during their disease course. However, before deploying this technique, numerous questions and challenges should be answered.

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