MUM1 expression dichotomizes follicular lymphoma into predominantly, MUM1-negative low-grade and MUM1-positive high-grade subtypes

doi:10.3324/haematol.10682

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Malignant Lymphomas

MUM1 expression dichotomizes follicular lymphoma into predominantly, MUM1-negative low-grade and MUM1-positive high-grade subtypes

Kikkeri N. Naresh

Department of Histopathology, Hammersmith Hospital & Imperial College, London, UK

Correspondence: Kikkeri N Naresh, Haematopathologist, Department of Histopathology, Hammersmith Hospital & Imperial College, Du Cane Road, W12 0HS, London UK. Phone: international +44.20.83833969. Fax: international +44.20.83838140. E-mail: k.naresh{at}imperial.ac.uk

ABSTRACT

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ABSTRACT
Acknowledgement
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We investigated the expression of MUM1 (multiple myeloma oncogene1)/IRF4 (interferon regulatory factor 4) in 46 cases of follicularlymphoma (FL) and correlated this with grade and expressionof CD10, Bcl-6 and Ki-67. The analysis suggests that MUM1 expressiondichotomizes FL into low-grade FL of CD10⁺/Bcl-6⁺/MUM1^–/Ki-67^lowpheno-type, and high-grade FL of CD10^+/–/Bcl-6^+/weak/MUM1⁺/Ki-67^highphenotype.

Key words: follicular lymphoma, MUM1, IRF4, Bcl-6, Bcl-2, CD10, Ki-67, germinal center, B-cell.

The MUM1 gene was first identified by cloning the chromosomalbreakpoints of a multiple myeloma cell line with translocationt(6;14)(p25;q32).¹ MUM1, a member of the IRF family of transcriptionalfactors, is induced by antigen receptor mediated stimuli andplays a crucial role in cell proliferation, differentiationand survival.

MUM1 is expresssed in plasma cells and in a small percentageof germinal center (GC) B cells mainly located in the lightzone. Most importantly, expression of MUM1 and Bcl-6 in GC Bcells appears to be mutually exclusive.² MUM1 is strongly expressedin multiple myeloma, lymphoplasmacytic lymphoma, classical Hodgkin’slymphoma, nearly one-half of diffuse large B-cell lymphomas(DLBCL), primary effusion lymphoma, immunoblastic lymphoma andplasmablastic lymphoma in the acquired immunodeficiency syndromesetting, post-transplant lymphoproliferative disorders, nearlyone-fifth of marginal zone lymphomas and a proportion of smalllymphocytic lymphomas. On the other hand it is said to be absentamong follicular lymphoma (FL) and mantle cell lymphoma. ^3–7

FL, a prototype GC B-cell lymphoma that expresses the GC markersCD10 and Bcl-6 is composed of centrocytes and centroblasts.FL is graded based on the number of centroblasts per high-power-field(hpf) and on the presence or absence of centrocytes.⁸ Gradingof FL and counting of centroblasts have high inter-observervariability. Furthermore, the distribution of centroblasts canbe heterogeneous. Hence additional ways of classifying FL needto be explored.

For the purposes of this study, 46 patients with FL, who hadbeen evaluated for expression of MUM1, CD10, Bcl-6 and Ki-67during routine diagnostic work-up, were selected. Twenty ofthe 46 cases were from the Hammersmith Hospital. The other 26cases were referrals. Immunohistochemical detection was performedusing MUM1 antibody (Santa Cruz Biotechnology Inc., USA). Forimmunohistochemical evaluation of Bcl-6, CD10 and MUM1, caseshad been scored ‘positive’ when at least 30% ofcells showed moderate to strong expression. With regards toKi-67 expression, the proportion of positive cells within theneoplastic follicles was estimated and expressed as a percentage.

Pearson’s ${chi}$ ² analysis was performed to correlate MUM1 expressionwith grade (grades 1 and 2 vs. grades 3a and 3b), expressionof CD10 and Bcl-6, and with the presence or absence of a DLBCLcomponent. An independent sample T-test was used to correlatethe difference in the mean Ki-67 expression between MUM1 positiveand negative groups.

Among the 46 cases, 12 had grade 1; 15 had grade 2; 9 had grade3a and 10 had grade 3b disease. Ten cases had an associatedDLBCL component. Seventeen cases (37%) were scored MUM1-positive.These cases showed moderate to strong expression in the nucleiin more than 30% of the cells within the follicles. Thirty-fivecases (76%) showed moderate to strong cytoplasmic membrane expressionof CD10. Forty-two cases (91.3%) showed moderate to strong Bcl-6expression. In the other four cases, Bcl-6 expression was weak(three cases) or focal (one case). None of the cases was completelynegative for Bcl-6 (Figure 1).

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Figure 1. A case of grade 1 follicular lymphoma with lack of MUM1 expression and a case of grade 3b follicular lymphoma showing easily appreciable MUM1 expression. The panel also shows differences in Ki-67 expression and a very similar expression of CD10 and Bcl-6 (all X200).

While 78.9% of FL of grades 3a and 3b were MUM1-positive, only7.4% of FL of grades 1 and 2 were MUM1-positive (p<0.0001).Nine of ten FL grade 3b FL (90%) were MUM1-positive. MUM1 expressionshowed a significant inverse correlation with CD10 and Bcl-6expression. Nine of 11 CD10-negative cases and all four casesin which Bcl-6 expression was weak were MUM1-positive (p<0.0001and p=0.006, respectively). Furthermore, MUM1-positive FL hada significantly higher proliferation/Ki-67 expression (56% inMUM1-positive cases vs. 26% in MUM1-negative cases; p<0.0001).

The first two papers on MUM1 expression in lymphomas suggestedthat FL are MUM1-negative.^2,3 However, in the study by Faliniet al., MUM1 expression was noted in 1/15 FL and the case wasin fact a grade 3 FL.² In a later publication, involving 50FL, 8% of grades 1 and 2 FL and 40% of grade 3 FL were foundto be MUM1-positive.⁹

Many studies have shown that tumor cells in DLBCL can co-expressMUM1 and Bcl-6.¹⁰ Based on CD10, Bcl-6 and MUM1 expression,DLBCL has been sub-classified into GC B-cell like and non-GCsubtypes. A high proportion of the non-GC subtype expressesMUM1 and this subtype is associated with a poor prognosis. Thecurrent study suggests a biological dichotomy among FL therebeing a low-grade FL with a CD10⁺/Bcl-6⁺/MUM1^–/Ki-67^lowphenotype and a high-grade FL with a CD10^+/–/Bcl-6^+/weak/MUM1^+/Ki-67^highphenotype.

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Table 1. Correlation of MUM1 expression with grade, expression of CD10, Bcl-6 and Ki-67, and presence of a DLBCL component.

	Acknowledgement

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I am most grateful for the cases sent for a second opinion thathave been included in the study: eight from Drs. Nayef Aqel& Gillian Williams (Northwick Park Hospital), seven fromDr. Graham Knee (Kingston Hospital), three from Drs. Mary Thompson& Alex Rice (St Mary’s Hospital), three from Drs.Fred Barker & Mike Williamson (Hillingdon Hospital), andone each from Dr. Margaret Burke (Harefield Hospital), Dr. Mohammed Al-Adnani (Ealing Hospital), Dr. Ann Thorpe (West MiddlesexUniversity Hospital), Dr. Phauda Thebe (Darrent Valley Hospital)and Dr. Madhuri Deolekar (North Manchester General Hospital)

References

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ABSTRACT
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References

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