Livin, a novel marker in lymphoma type distinction.

[hodgkin lymphoma, classical]

Despite advances in immunohistochemical and molecular diagnostics , there are persistent difficulties in differentiating between several subtypes of non-Hodgkin lymphoma (NHL ) and classic Hodgkin lymphoma (CHL ). Considering high level of livin expression in hematologic malignancies , we aimed to examine the utility of livin expression ratio , as an ancillary biomarker , in distinguishing CHL from NHL in ambiguous cases . We evaluated livin expression in 38 CHL , 23 NHL , and 39 nonneoplastic lymph nodes in paraffin-embedded blocks . Tissue microarray-based semiquantitative immunoflourecent staining was applied for protein expression . Criterion standard of diagnosis was based on selection of only definite cases and not the cases suspected by hemathopathologists . A significant difference was found in the livin /GAPDH mean ratio (M .R ) of expression between NHL and CHL cases . A receiver operating characteristic curve analysis confirmed 0 .6370 to be the best diagnostic cut-off value for the livin /GAPDH expression M .R in diffuse large B-cell lymphoma (DLBCL ) (area under the curve = 0 .944 ); it yielded 92 % sensitivity , 94 % specificity , likelihood ratios positive 17 .5 , and likelihood ratios negative 0 .07 for diagnosing DLBCL from CHL . Mean ratio of livin /Glyceraldehyde 3 -phosphate dehydrogenase (GAPDH ) expression seems to be a valuable index in differentiating DLBCL from CHL . We suggested an optimal cut-off point for livin /GAPDH expression M .R with a high sensitivity and specificity . Thus , in diagnostically difficult cases of DLBCL and CHL , focus on livin as marker may provide useful corroborative information .