Genomic heterogeneity of ALK fusion breakpoints in non-small-cell lung cancer.
Jason N RosenbaumRyan BloomJason T ForysJeff HikenJon R ArmstrongJulie BransonSamantha McNultyPriya D VeluKymberlie PepinHaley AbelCatherine E CottrellJohn D PfeiferShashikant KulkarniRamaswamy GovindanEric Q KonnickChristina M LockwoodEric J DuncavagePublished in: Modern pathology : an official journal of the United States and Canadian Academy of Pathology, Inc (2018)
In lung adenocarcinoma, canonical EML4-ALK inversion results in a fusion protein with a constitutively active ALK kinase domain. Evidence of ALK rearrangement occurs in a minority (2-7%) of lung adenocarcinoma, and only ~60% of these patients will respond to targeted ALK inhibition by drugs such as crizotinib and ceritinib. Clinically, targeted anti-ALK therapy is often initiated based on evidence of an ALK genomic rearrangement detected by fluorescence in situ hybridization (FISH) of interphase cells in formalin-fixed, paraffin-embedded tissue sections. At the genomic level, however, ALK rearrangements are heterogeneous, with multiple potential breakpoints in EML4, and alternate fusion partners. Using next-generation sequencing of DNA and RNA together with ALK immunohistochemistry, we comprehensively characterized genomic breakpoints in 33 FISH-positive lung adenocarcinomas. Of these 33 cases, 29 (88%) had detectable DNA level ALK rearrangements involving EML4, KIF5B, or non-canonical partners including ASXL2, ATP6V1B1, PRKAR1A, and SPDYA. A subset of 12 cases had material available for RNA-Seq. Of these, eight of eight (100%) cases with DNA rearrangements showed ALK fusion transcripts from RNA-Seq; three of four cases (75%) without detectable DNA rearrangements were similarly negative by RNA-Seq, and one case was positive by RNA-Seq but negative by DNA next-generation sequencing. By immunohistochemistry, 17 of 19 (89%) tested cases were clearly positive for ALK protein expression; the remaining cases had no detectable DNA level rearrangement or had a non-canonical rearrangement not predicted to form a fusion protein. Survival analysis of patients treated with targeted ALK inhibitors demonstrates a significant difference in mean survival between patients with next-generation sequencing confirmed EML4-ALK rearrangements, and those without (20.6 months vs 5.4 months, P<0.01). Together, these data demonstrate abundant genomic heterogeneity among ALK-rearranged lung adenocarcinoma, which may account for differences in treatment response with targeted ALK inhibitors.
Keyphrases
- rna seq
- advanced non small cell lung cancer
- single cell
- circulating tumor
- copy number
- epidermal growth factor receptor
- single molecule
- cell free
- cancer therapy
- magnetic resonance imaging
- computed tomography
- end stage renal disease
- dna methylation
- magnetic resonance
- bone marrow
- chronic kidney disease
- mesenchymal stem cells
- risk assessment
- machine learning
- tyrosine kinase
- patient reported outcomes
- contrast enhanced
- circulating tumor cells
- genome wide
- hepatitis c virus