Clinicopathologic Consensus Study of Gray Zone Lymphoma with Features Intermediate Between DLBCL and Classical HL

Overview

Journal Blood Adv

Specialty Hematology

Date 2018 Jan 4

PMID 29296913

Citations 27

Authors

Monika Pilichowska

Stefania Pittaluga

Judith A Ferry

Jessica Hemminger

Hong Chang

Jennifer A Kanakry

Laurie H Sehn

Tatyana Feldman

Jeremy S Abramson

Athena Kritharis

Francisco J Hernandez-Ilizaliturri

Izidore S Lossos

Oliver W Press

Timothy S Fenske

Jonathan W Friedberg

Julie M Vose

Kristie A Blum

Deepa Jagadeesh

Bruce Woda

Gaurav K Gupta

Randy D Gascoyne

Elaine S Jaffe

Andrew M Evens

Affiliations

Soon will be listed here.

Abstract

Gray zone lymphoma (GZL) is described as sharing features with classical Hodgkin lymphoma (cHL) and diffuse large B-cell lymphoma (DLBCL). However, there remains complexity in establishing diagnosis, delineating prognosis, and determining optimum therapy. Sixty-eight cases diagnosed as GZL across 15 North American academic centers were evaluated by central pathology review to achieve consensus. Of these, only 26 (38%) were confirmed as GZL. Morphology was critical to GZL consensus diagnosis (eg, tumor cell richness); immunohistochemistry showed universal B-cell derivation, frequent CD30 expression, and rare Epstein-Barr virus (EBV) positivity (CD20, 83%; PAX5, 100%; BCL6, 20%; MUM1, 100%; CD30, 92%; EBV, 4%). Forty-two cases were reclassified: nodular sclerosis (NS) cHL, n = 27 (including n = 10 NS grade 2); lymphocyte predominant HL, n = 4; DLBCL, n = 4; EBV DLBCL, n = 3; primary mediastinal large BCL n = 2; lymphocyte-rich cHL and BCL-not otherwise specified, n = 1 each. GZL consensus-confirmed vs reclassified cases, respectively, more often had mediastinal disease (69% vs 41%; .038) and less likely more than 1 extranodal site (0% vs 25%; .019). With a 44-month median follow-up, 3-year progression-free survival (PFS) and overall survival for patients with confirmed GZL were 39% and 95%, respectively, vs 58% and 85%, respectively, for reclassified cases ( .19 and .15, respectively). Interestingly, NS grade 2 reclassified patients had similar PFS as GZL consensus-confirmed cases. For prognostication of GZL cases, hypoalbuminemia was a negative factor (3-year PFS, 12% vs 64%; = .01), whereas frontline cyclophosphamide, doxorubicin, vincristine, and prednisone ± rituximab (CHOP±R) was associated with improved 3-year PFS (70% vs 20%; .03); both factors remained significant on multivariate analysis. Altogether, accurate diagnosis of GZL remains challenging, and improved therapeutic strategies are needed.

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