Ultra-Deep Sequencing Reveals the Mutational Landscape of Classical Hodgkin Lymphoma

Author:

Gomez FeliciaORCID,Mosior Matthew,McMichael JoshuaORCID,Skidmore Zachary L.,Duncavage Eric J.ORCID,Miller Christopher A.ORCID,Abel Haley J.,Li Yi-Shan,Krysiak KilanninORCID,Russler-Germain David A.ORCID,Watkins Marcus P.,Ramirez CodyORCID,Schmidt AlinaORCID,Rodrigues Fernanda MartinsORCID,Trani Lee,Khanna Ajay,Wagner Julia A.ORCID,Fulton Robert S.,Fronick Catrina,O’Laughlin Michelle,Schappe Timothy,Cashen Amanda,Mehta-Shah Neha,Kahl Brad S.ORCID,Walker Jason,Bartlett Nancy L.ORCID,Griffith MalachiORCID,Fehniger Todd A.ORCID,Griffith Obi L.ORCID

Abstract

AbstractThe malignant Hodgkin and Reed Sternberg (HRS) cells of classical Hodgkin lymphoma (cHL) are scarce in affected lymph nodes, creating a challenge to detect driver somatic mutations. As an alternative to cell purification techniques, we hypothesized that ultra-deep exome sequencing would allow genomic study of HRS cells, thereby streamlining analysis and avoiding technical pitfalls. To test this, 31 cHL tumor/normal pairs were exome sequenced to ∼1000x median depth of coverage. An orthogonal error-corrected sequencing approach verified >95% of the discovered mutations. We identified mutations in genes novel to cHL including: CDH5 and PCDH7; novel mutations in IL4R, and a novel pattern of recurrent mutations in pathways regulating Hippo signaling. This study provides proof-of-principle that ultra-deep exome sequencing can be utilized to identify recurrent mutations in HRS cells, allowing for the analysis for clinically relevant genomic variants in large cohorts of cHL patients.

Publisher

Cold Spring Harbor Laboratory

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