Discriminating lymphomas and reactive lymphadenopathy in lymph node biopsies by gene expression profiling

A Rosenwald; A Sanchez-Aguilera; AA Alizadeh; AC Seegmiller; Adam Bryant; AN Schuetz; Anna Campain; CH Lawrie; CP Hans; David DF Ma; IS Lossos; JB Welsh; Jennifer Turner; JJ Turner; KJ Savage; L Belov; L Ein-Dor; LJ van't Veer; LM Rimsza; M Jung; M Niens; MA Shipp; Mark Lutherborrow; O Bereczki; P Farinha; R Schmitz; RL Somorjai; S Blenk; S Monti; SS Dave; Tim J Molloy; To Ha Loi; U Alon; Y Natkunam; Yee Hwa Jean Yang; YH Yang

Discriminating lymphomas and reactive lymphadenopathy in lymph node biopsies by gene expression profiling

Authors: A Rosenwald
A Sanchez-Aguilera
AA Alizadeh
AC Seegmiller
Adam Bryant
AN Schuetz
Anna Campain
CH Lawrie
CP Hans
David DF Ma
IS Lossos
JB Welsh
Jennifer Turner
JJ Turner
KJ Savage
L Belov
L Ein-Dor
LJ van't Veer
LM Rimsza
M Jung
M Niens
MA Shipp
Mark Lutherborrow
O Bereczki
P Farinha
R Schmitz
RL Somorjai
S Blenk
S Monti
SS Dave
Tim J Molloy
To Ha Loi
U Alon
Y Natkunam
Yee Hwa Jean Yang
YH Yang
Publication date: 1 January 2011
Publisher: BioMed Central
Doi

Abstract

Abstract Background Diagnostic accuracy of lymphoma, a heterogeneous cancer, is essential for patient management. Several ancillary tests including immunophenotyping, and sometimes cytogenetics and PCR are required to aid histological diagnosis. In this proof of principle study, gene expression microarray was evaluated as a single platform test in the differential diagnosis of common lymphoma subtypes and reactive lymphadenopathy (RL) in lymph node biopsies. Methods 116 lymph node biopsies diagnosed as RL, classical Hodgkin lymphoma (cHL), diffuse large B cell lymphoma (DLBCL) or follicular lymphoma (FL) were assayed by mRNA microarray. Three supervised classification strategies (global multi-class, local binary-class and global binary-class classifications) using diagonal linear discriminant analysis was performed on training sets of array data and the classification error rates calculated by leave one out cross-validation. The independent error rate was then evaluated by testing the identified gene classifiers on an independent (test) set of array data. Results The binary classifications provided prediction accuracies, between a subtype of interest and the remaining samples, of 88.5%, 82.8%, 82.8% and 80.0% for FL, cHL, DLBCL, and RL respectively. Identified gene classifiers include LIM domain only-2 (<it>LMO2</it>), Chemokine (C-C motif) ligand 22 (<it>CCL22</it>) and Cyclin-dependent kinase inhibitor-3 (<it>CDK3</it>) specifically for FL, cHL and DLBCL subtypes respectively. Conclusions This study highlights the ability of gene expression profiling to distinguish lymphoma from reactive conditions and classify the major subtypes of lymphoma in a diagnostic setting. A cost-effective single platform "mini-chip" assay could, in principle, be developed to aid the quick diagnosis of lymph node biopsies with the potential to incorporate other pathological entities into such an assay.</p