This Article Abstract Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Email this article to a friend Similar articles in this journal Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via HighWire Citing Articles via ISI Web of Science (1) Citing Articles via Google Scholar Google Scholar Articles by Ramos-Vara, J. A. Articles by Valli, V. E. O. Search for Related Content PubMed Articles by Ramos-Vara, J. A. Articles by Valli, V. E. O. Social Bookmarking                            What's this?

Immunohistochemical Detection of Multiple Myeloma 1/Interferon Regulatory Factor 4 (MUM1/IRF-4) in Canine Plasmacytoma: Comparison with CD79a and CD20

Animal Disease Diagnostic Laboratory and Department of Comparative Pathobiology, School of Veterinary Medicine, Purdue University, West Lafayette, Indiana (JAR, MAM), Department of Pathobiology, College of Veterinary Medicine, University of Illinois, Urbana, IL (VEV)

	Abstract

Top Abstract Methods Results Discussion Acknowledgement References

 
Multiple myeloma oncogene 1/interferon regulatory factor 4 (MUM1/IRF4) is involved in lymphoid cell differentiation, particularly in the production of plasma cells. We examined the immunoreactivity of mouse monoclonal antibody Mum-1p to MUM1/IRF4 and compared it with expression of CD79a and CD20 in 109 plasmacytomas in 107 dogs. Tissues had been fixed in formalin and embedded in paraffin. One hundred one of 109 (93.5%) tumors were positive for MUM1/IRF4. The staining was nuclear with weak cytoplasmic reaction. Fifty-nine of 105 (56.2%) plasmacytomas were positive for CD79a; only 21 of 108 (19.4%) cases were positive for CD20. MUM1/IRF4 staining was performed on 139 other tumors including B- and T-cell lymphomas, histiocytic proliferations, mast cell tumors, and melanocytic tumors. The only MUM1/IRF4-positive nonplasmacytic tumors were 10 B-cell lymphomas and 1 anaplastic lymphoma. We conclude the following: 1) Antibody Mum-1p is very specific for canine plasmacytomas, 2) antibody Mum-1p is superior in sensitivity and specificity to CD79a and CD20 for the identification of canine plasmacytomas in formalin-fixed, paraffin-embedded tissues, 3) canine lymphomas that express MUM1/IRF4 are few and usually of B-cell origin, 4) other canine leukocytic and melanocytic tumors do not express MUM1/IRF4, and 5) prospective studies are needed to determine whether the expression of MUM1/IRF4, particularly in lymphomas, has prognostic significance.

Key words: CD20; CD79a; dogs; immunohistochemistry; lymphoma; MUM1/IRF4; pathology; plasmacytoma.

Extramedullary plasmacytomas (EMPs) are neoplasms of plasma cells at varying stages of differentiation that do not involve bone.²⁵ EMPs are uncommon in dogs and usually affect the skin, constituting 1.5% of all cutaneous neoplasms.¹⁸ Cutaneous plasmacytomas also have been recognized in cats and horses.^20,32 Most cutaneous plasmacytomas are solitary; multiple lesions are uncommon.²⁰ Typical locations of cutaneous plasmacytomas are the pinnae, lips, digits, and chin.²⁰ Cutaneous plasmacytomas are observed mainly in adult and geriatric dogs.²⁰ Most canine cutaneous plasmacytomas have benign behavior, although rarely they involve viscera, including bone marrow.³⁰ Plasmacytomas can affect other organs or tissues including the oral cavity, intestine (particularly the rectum), liver, spleen, kidney, lung, and brain.^25,42,43 Canine plasmacytomas have been classified histologically as 5 types: mature, hyaline, cleaved, asynchronous, and polymorphous-blastic.³⁷ An additional type, monomorphous-blastic, has been included by other authors.⁵ Multiple myeloma (MM), a tumor of plasma cells involving at least the bone marrow, is rarer than extramedullary plasmacytoma and has been reported in dogs, cats, cattle, horses, and pigs.²⁵ Human EMPs are rare, typically solitary tumors found in the upper respiratory tract and less commonly in the gastrointestinal and genitourinary tracts, lungs, lymph nodes, and skin.²⁸ Human EMPs have an indolent course, with frequent local recurrence; conversion to MM may occur.^28,56

Plasmacytoma is a tumor of monoclonal immunoglobulin-producing cells, so diagnosis was initially based on immunohistochemical demonstration of cytoplasmic immunoglobulins, particularly clonality for or light chains of immunoglobulins.^20,42 Canine plasmacytomas are also positive for CD45 and immunoglobulins G, A, or M and variably express CD18, CD45RA, and CD79a leukocytic antigens.^15,20,42 CD79a, a molecule of the B-cell antigen receptor complex that is expressed from the pre–pre-B-cell stage to the plasma cell differentiation stage,²³ has been detected in more than 60% of human EMPs and the majority of MMs.²⁸ In dogs, CD79a is expressed in up to 80% of plasmacytomas.^20,46 CD20, a transmembrane phosphoprotein predominantly expressed from the pre-B cell stage to the activated B-cell stage,²³ has been detected immunohistochemically in normal canine B cells and lymphomas²⁶; however, CD20 reactivity in normal or neoplastic plasma cells has not been reported. Many more markers are used in human medicine than in veterinary medicine. Currently, markers used in the characterization of human EMPs and MMs in formalin-fixed, paraffin-embedded tissues include antibodies to Blimp-1, CD20, CD38, CD56, CD 138/syndecan-1, multiple myeloma oncogene 1/interferon regulatory factor 4 (MUM1/IRF4), and antibody VS38c.^{7,19,28,44,47,51}

Interferon regulatory factors (IRFs) are a family of transcription factors involved in regulation of cell growth and immunologic responses.³¹ MUM1, also called IRF4, is involved in lymphoid cell differentiation.¹⁶ MUM1/IRF4 is required for immunoglobulin light-chain rearrangement at the pre–B stage of lymphocyte maturation.³³ MUM1/IRF4 is expressed in a subset of germinal center B cells, plasma cells, activated T cells, and a subset of macrophages and dendritic cells.^{3,10,14,50,52} MUM1/IRF4-deficient mice do not form germinal centers, lack plasma cells, and have markedly reduced serum immunoglobulin.³⁴ MUM1/IRF4 antibodies are used as part of an immunohistochemical panel to characterize human B-cell neoplasms. MUM1 is expressed in diffuse large B-cell lymphoma of postgerminal center (CD10^–/bcl-6^±/MUM1⁺/CD138^–) and plasmablastic (CD10^–/bcl-6^–/MUM1⁺/CD138⁺) origins.^10,17,52 In classic Hodgkin's lymphoma, MUM1/IRF4 is detected in Hodgkin's lymphoma Reed-Sternberg cells.^6,36,52 MUM1/IRF4 is expressed in the majority of cutaneous plasmacytomas and multiple myelomas.^36,52 Human T-cell lymphomas, including adult T-cell leukemia lymphoma and anaplastic large cell lymphoma, are frequently MUM1/IRF4-positive.⁵² The only reported nonleukocytic human tumor expressing MUM1 is melanoma.^36,48 MUM1/IRF4 has been used as a prognostic factor in different studies. MUM1/IRF4 expression correlates with unfavorable prognosis in B-cell chronic lymphocytic leukemia/small lymphocytic lymphoma^8,24 and probably in diffuse large B-cell lymphoma,^21,22 although other reports could not find such correlation.^2,10 In primary cutaneous B-cell lymphomas, MUM1/IRF4 expression is associated with reduced survival times.⁴⁹ To our knowledge, the expression of MUM1/IRF4 has not been reported in dogs or other domestic species. The objectives of this study were the following: 1) immunohistochemical detection of MUM1/IRF4 with monoclonal antibody Mum-1p in canine plasmacytomas, 2) comparison of results of immunohistochemical expression of MUM1/IRF4 with that of CD20 and CD79a in canine plasmacytomas, and 3) evaluation of the immunohistochemical staining for MUM1/IRF4 in canine leukocytic and melanocytic tumors.

	Methods

Top Abstract Methods Results Discussion Acknowledgement References

 
Case material came from the archives of the Animal Disease Diagnostic Laboratory-Purdue University and the Department of Pathobiology-University of Illinois. A total of 109 plasmacytomas from 107 dogs were examined (Table 1). These tumors were mostly cutaneous (80) with fewer from the oral cavity (18), rectum (4), spleen (2), lung (1), brain (1), liver (1), and bone marrow (1). Plasmacytomas were histologically classified according to Platz et al.³⁷ We also evaluated antibody Mum-1p reactivity in 139 other tumors, including lymphoid proliferations (89), histiocytic proliferations (31), mast cell tumors (7), and melanocytic tumors (13).

	Results

Top Abstract Methods Results Discussion Acknowledgement References

View larger version (211K): [in this window] [in a new window]   Fig. 1. Skin; dog. Plasmacytoma, polymorphous type. HE. Bar = 40 µm. Fig. 2. Skin; dog. Plasmacytoma, cleaved type. HE. Bar = 20 µm. Fig. 3. Skin; dog. Plasmacytoma, hyaline type. HE. Bar = 40 µm. Fig. 4. Skin; dog. Plasmacytoma, asynchronous type. HE. Bar = 40 µm. Fig. 5. Skin; dog. Plasmacytoma, mature type. Plasma cells are surrounded by amyloid and foreign body multinucleated giant cells (asterisk). HE. Bar = 40 µm. Fig. 6. Skin; dog. Plasmacytoma. The dermis is diffusely infiltrated by neoplastic cells. Strong staining with Mum-1p antibody. Immunoperoxidase for multiple myeloma oncogene 1/interferon regulatory factor 4, Mayer's hematoxylin counterstain, HE. Bar = 400 µm. Fig. 7. Skin; dog. Plasmacytoma. Detail of staining with antibody Mum-1p. Strong nuclear and weak cytoplasmic staining in most cells. Bar = 40 µm. Upper inset: Staining of multinucleated giant cell. Lower inset: Staining of binucleated giant cell. Immunoperoxidase for multiple myeloma oncogene 1/interferon regulatory factor 4, Mayer's hematoxylin counterstain. Bar = 20 µm.

View larger version (213K): [in this window] [in a new window]   Fig. 8. Rectum; dog. Plasmacytoma. Neoplastic cells in the lamina propria (lp) and submucosa (s) are positive. Immunoperoxidase for multiple myeloma oncogene 1/interferon regulatory factor 4, Mayer's hematoxylin counterstain. Bar = 400 µm. Fig. 9. Rectum; dog. Plasmacytoma. Numerous variably stained cells are interspersed among mucosal glands. Immunoperoxidase for multiple myeloma oncogene 1/interferon regulatory factor 4, Mayer's hematoxylin counterstain. Bar = 80 µm. Fig. 10. Skin; dog. Plasmacytoma. Distinct cytoplasmic membrane staining in numerous cells. Immunoperoxidase for CD20, Mayer's hematoxylin counterstain. Bar = 40 µm. Fig. 11. Tonsil; dog. Fig. 11A. Diffuse large cell B-cell lymphoma, immunoblastic type. The neoplastic growth involves mainly the deep tissues (s) and contains numerous positive cells. Normal follicles (f) and interfollicular areas have occasional positive cells. Bar = 400 µm. Fig. 11B. Nuclear staining is variable within this tumor. Immunoperoxidase for multiple myeloma oncogene 1/interferon regulatory factor 4, Mayer's hematoxylin counterstain. Bar = 40 µm. Fig. 12. Lymph node; dog. Follicular lymphoma. Many neoplastic lymphocytes react with antibody Mum-1p. A thin rim of nonneoplastic lymphocytes in the periphery of the follicles has rare positive cells (arrows). Immunoperoxidase for multiple myeloma oncogene 1/interferon regulatory factor 4, Mayer's hematoxylin counterstain. Bar = 160 µm. Fig. 13. Intestine; dog. Anaplastic large cell lymphoma. Diffuse staining in the lamina propria (lp) and submucosa (s). Immunoperoxidase for multiple myeloma oncogene 1/interferon regulatory factor 4, Mayer's hematoxylin counterstain. Bar = 400 µm.

	Discussion

Top Abstract Methods Results Discussion Acknowledgement References

 
The most common histologic forms of plasmacytomas in our series were cleaved and asynchronous. These 2 forms are reportedly the most common canine plasmacytoma types.³⁷ Histologic grading of canine plasmacytomas does not seem to correlate with biologic behavior, which usually is benign.^1,37 In our series, only 2 cases involved multiple organs, and neither of these had cutaneous lesions. Although follow-up attempts were not made, we did not find in the databases used in this study evidence of recurrence of the tumors. Amyloid is observed in about 10% of canine plasmacytomas²⁰; a similar percentage of cases with amyloid deposition was present in our series. The mean age of presentation of plasmacytomas was 9.4 years, similar to the 9.2 years reported in another large study¹⁸ in which the head was the site most frequently involved; however, in the current study, the most common location was the leg. Most human EMPs are in the upper respiratory tract, oral cavity, or gastrointestinal tract.^9,27 Human cutaneous plasmacytomas are rare and usually solitary; visceral metastases or progression to multiple myeloma is observed in one third of cases.^56,57

Immunohistochemical detection of immunoglobulin heavy and light chains has been the standard test for plasma cell differentiation.^{1,4,5,13,29,35,38,42,45} However, nonspecific staining may result from adsorption of immunoglobulins to the cell surface, internalization by phagocytes, or binding of immunoglobulins to a variety of cell types via Fc receptors.⁴⁶ Although reactivity of CD79a in canine plasmacytoma and B-cell lymphomas is well established, there are large variations in the percentage of cases and number of cells stained with this marker, with up to 80% of plasmacytomas expressing CD79a.^20,42,46

To our knowledge, this is the first report of MUM1/IRF4 immunohistochemical detection in canine plasmacytomas and other canine round cell tumors. In addition, we compared reactivity of MUM1/IRF4 with that for other B-cell markers, CD79a and CD20, in a large series of canine plasmacytomas. More than 94% of canine plasmacytomas were positive for MUM1/IRF4. Two of the negative cases were digital lesions that had been decalcified; these cases were also negative for CD79a and CD20, which suggests the possibility that decalcification hindered immunohistochemical detection of these antigens. This was a retrospective study, and no attempts were made to determine the significance of expression of MUM1/IRF4 in canine plasmacytomas and lymphomas. In humans, MUM1/IRF4 expression correlates with unfavorable outcome or decreased survival in B-cell chronic lymphocytic leukemia/small lymphocytic lymphoma, diffuse large B-cell lymphoma, and primary cutaneous B-cell lymphomas^{8,21,22,24,29}; other investigators could not find such correlation.^2,10 Although MUM1/IRF4 is typically expressed in postgerminal center lymphomas,¹⁰ 2 of the 10 B-cell lymphomas that were positive for this marker were high-grade follicular lymphoma.

In the current study, the number of CD79a-positive plasmacytomas was markedly lower than that for MUM1/IRF4. This was not unexpected considering the reported expression of CD79a during lymphoid maturation.²³ CD79a is expressed from the pre–pre-B-cell stage to the plasma cell stage, but it is not expressed in all plasma cells and their tumors.¹⁹ However, other authors reported 13 of 16 canine plasmacytomas positive for CD79a.⁴⁶ This discrepancy could reflect differences in scoring criteria.

Of the 3 B-cell markers used in this study, CD20 was the least likely to be expressed in canine plasmacytomas. CD20 is expressed from the pre–B-cell stage to the activated B-cell stage²³ and is not detected in human EMPs or multiple myelomas, although a few normal plasma cells can show reactivity.^9,27,28,55 Typically, human plasmacytomas have a MUM1/IRF4⁺, CD79a⁺, CD20^– immunophenotype, with expression of other markers such as CD138 and VS38c.^{7,19,28,44,51,55} Our results correlate fairly well with those of the human literature, particularly for MUM1/IRF4 and CD20. We did not find references of CD20 reactivity in canine plasmacytomas.

Specificity of the antibody Mum-1p for plasma cells and their tumors was evaluated by examining its reactivity in other leukocytic and melanocytic tumors because some T- and B-cell lymphomas, in addition to melanomas, have been reported to express MUM1/IRF4 in humans.^6,36,52 Only 10 B-cell lymphomas and 1 anaplastic lymphoma from a total of 139 leukocytic and melanocytic neoplasms expressed MUM1/IRF4. In our series, diffuse large cell B-cell lymphoma was the most common nonplasmacytic tumor to express MUM1/IRF4. None of the marginal zone lymphomas in our series (6 nodal, 1 splenic) were positive for MUM1/IRF4. We did not observe plasmacytic differentiation in these tumors, but some human extranodal marginal zone lymphomas have this differentiation and MUM1/IRF4 is the most commonly expressed plasma cell marker.^11,12 A result that deserves further examination is the strong detection of MUM1/IRF4 in centrocytes in a single case of advanced or late-stage (III) follicular lymphoma (FL). Currently FL is identified on oversight staining by a tissue architecture with tightly facetted and coalescing follicles that have lost most or all of the mantle cell cuffs and have a uniform population of cells across the follicular diameter.⁵⁴ In contrast, nodes with even atypical follicular hyperplasia retain an antigen-related polarity most evident in those centers immediately beneath the node capsule. This polarity is characterized by segregation of cells with centroblastic nuclei into the deep or dark pole area and those with centrocytic nuclei into the superficial or light-pole area. Since most follicular center cells stain positively with B-cell markers in both benign and neoplastic follicles, the availability of a stain that marked only the centrocytes of neoplastic follicles would be a valuable addition to animal diagnostic hematopathology. However, this finding needs to be confirmed using a larger series of FL. In humans, up to 95% of melanomas express MUM1/IRF4.^36,48 We examined canine oral melanomas and cutaneous melanocytomas, and none showed reactivity for antibody Mum-1p.

Although other nonleukocytic tumors were not examined in our series, these results indicate the following: 1) Antibody Mum-1p is very specific for canine plasmacytomas, 2) antibody Mum-1p is superior in sensitivity and specificity to CD79a and CD20 for the detection of canine plasmacytomas in formalin-fixed, paraffin-embedded tissues, 3) the sensitivity of antibody Mum-1p to detect canine plasmacytomas was 93.5%; when combined with CD79a, it increased to 95.5%, 4) few canine lymphomas, usually of B-cell origin, express MUM1/IRF4, 5) canine melanomas and other leukocytic tumors do not express MUM1/IRF4, and 6) prospective studies are needed to determine whether the expression of MUM1/IRF4, particularly in lymphomas, has prognostic significance.

	Acknowledgement

Top Abstract Methods Results Discussion Acknowledgement References

 
We appreciate the technical expertise of Dee DuSold in performing immunohistochemistry.

	References

Top Abstract Methods Results Discussion Acknowledgement References

 

1. Baer KE, Patnaik AK, Gilbertson SR, Hurvitz AI. Cutaneous plasmacytomas in dogs: a morphologic and immunohistochemical study. Vet Pathol 26:216–221, 1989[Abstract]
2. Berglund M, Thunberg U, Amini R, Book M, Roos G, Erlanson M, Linderoth J, Dictor M, Jerkeman M, Cavallin-Ståhl E, Sundström C, Rehn-Eriksson S, Backlin C, Hagberg H, Rosenquist R, Enblad G. Evaluation of immunophenotype in diffuse large B-cell lymphoma and its impact on prognosis. Mod Pathol 18:1113–1120, 2005[CrossRef][Web of Science][Medline]
3. Brighenti A, Andrulis M, Geissinger E, Roth S, Müller-Hermelink HK, Rüdiger T. Extrafollicular proliferation of B cells in the absence of follicular hyperplasia: a distinct reaction pattern in lymph nodes correlated with primary or recall type responses. Histopathology 47:90–100, 2005[CrossRef][Web of Science][Medline]
4. Brunnert SR, Altman NH. Identification of immunoglobulin light chains in canine extramedullary plasmacytomas by thioflavine T and immunohistochemistry. J Vet Diagn Invest 3:245–251, 1991[Abstract/Free Full Text]
5. Cangul IT, Wijnen M, van Garderen E, van den Ingh TSGAM. Clinico-pathological aspects of canine cutaneous and mucocutaneous plasmacytomas. J Vet Med A Physiol Pathol Clin Med 49:307–312, 2002[Medline]
6. Carbone A, Gloghini A, Aldinucci D, Gattei V, Dalla-Favera R, Gaidano G. Expression pattern of MUM1/IRF4 in the spectrum of pathology of Hodgkin's disease. Br J Haematol 117:366–372, 2002[CrossRef][Web of Science][Medline]
7. Cattoretti G, Angelin-Duclos C, Shaknovich R, Zhou H, Wang D, Alobeid B. PRDMI/Blimp-I is expressed in human B-lymphocytes committed to the plasma cell lineage. J Pathol 206:76–86, 2005[CrossRef][Web of Science][Medline]
8. Chang C, Lorek J, Sabath DE, Li Y, Chitambar CR, Logan B, Kampalath B, Cleveland RP. Expression of MUM1/IRF4 correlates with clinical outcome in patients with B-cell chronic lymphocytic leukemia. Blood 100:4671–4675, 2002[Abstract/Free Full Text]
9. Chen T-C, Wu J-H, Ng K-F, Lien J-M, Hung C-F. Solitary extramedullary plasmacytoma in the retroperitoneum. Am J Hematol 58:235–238, 1998[CrossRef][Web of Science][Medline]
10. Colomo L, López-Guillermo A, Perales M, Rives S, Martínez A, Bosch F, Colomer D, Falini B, Montsserrat E, Campo E. Clinical impact of the differentiation profile assessed by immunophenotyping in patients with diffuse large B-cell lymphoma. Blood 101:78–84, 2003[Abstract/Free Full Text]
11. Coupland SE, Foss H-D, Hidayat AA, Cockerham GC, Hummel M, Stein H. Extranodal marginal zone B cell lymphomas of the uvea: an analysis of 13 cases. J Pathol 197:333–340, 2002[CrossRef][Web of Science][Medline]
12. Coupland SE, Hellmich M, Auw-Haedrich C, Lee WR, Anagnostopoulos I, Stein H. Plasmacellular differentiation in extranodal marginal zone B cell lymphomas of the ocular adnexa: an analysis of the neoplastic plasma cell phenotype and its prognostic significance in 136 cases. Br J Ophthalmol 89:352–359, 2005[Abstract/Free Full Text]
13. Day MJ. Immunophenotypic characterization of cutaneous lymphoid neoplasia in the dog and cat. J Comp Pathol 112:79–96, 1995[CrossRef][Web of Science][Medline]
14. Falini B, Fizzotti M, Pucciarini A, Bigerna B, Marafioti T, Gambacorta M, Pacini R, Alunni C, Natali-Tanci L, Ugolini B, Sebastiani C, Cattoretti G, Pileri S, Dalla-Favera R, Stein H. A monoclonal antibody (MUM1p) detects expression of the MUM1/IRF4 protein in a subset of germinal center B cells, plasma cells, and activated T cells. Blood 95:2084–2092, 2000[Abstract/Free Full Text]
15. Fernandez NJ, West KH, Jackson ML, Kidney BA. Immunohistochemical and histochemical stains for differentiating canine cutaneous round cell tumors. Vet Pathol 42:437–445, 2005[Abstract/Free Full Text]
16. Gaidano G, Carbone A. MUM1: a step ahead toward the understanding of lymphoma histogenesis. Leukemia 14:563–566, 2000[CrossRef][Web of Science][Medline]
17. Gaidano G, Cerri M, Capello D, Berra E, Deambrogi C, Rossi D, Larocca LM, Campo E, Gloghini A, Tirelli U, Carbone A. Molecular histogenesis of plasmablastic lymphoma of the oral cavity. Br J Haematol 119:622–628, 2002[CrossRef][Web of Science][Medline]
18. Goldschmidt MH, Shofer FS. Cutaneous plasmacytomas. In: Skin Tumors of the Dog and Cat Goldschmidt MH, Shofer FS, eds. 265–270,Pergamon Press, Oxford, UK. 1992
19. Grogan TM, Van Camp B, Kyle RA. Plasma cell neoplasms. In: Pathology and Genetics of Tumors of Haematopoietic and Lymphoid Tissues Jaffe ES, Harris NL, Stein H, Vardiman JW, eds. 142–156,IARC Press, Lyon, France. 2001
20. Gross TL, Ihrke PJ, Walder EJ, Affolter VK. Cutaneous plasmacytoma. In: Skin Diseases of the Dog and Cat: Clinical and Histopathologic Diagnosis Gross TL, Ihrke PJ, Walder EJ, Affolter VK, eds. 2nd ed., 866–872,Blackwell Science, Oxford, UK. 2005
21. Haarer CF, Roberts RA, Frutiger YM, Grogan TM, Rimsza LM. Immunohistochemical classification of de novo, transformed, and relapsed diffuse large B-cell lymphoma into germinal center B-cell and nongerminal center B-cell subtypes correlates with gene expression profile and patient survival. Arch Pathol Lab Med 130:1819–1824, 2006[Web of Science][Medline]
22. Hans CP, Weisenburger DD, Greiner TC, Gascoyne RD, Delabie J, Ott G, Müller-Hermelink HK, Campo E, Braziel RM, Jaffe ES, Pan Z, Farinha P, Smith LM, Falini B, Banham AH, Rosenwald A, Staudt LM, Connors JM, Armitage JO, Chan WC. Confirmation of the molecular classification of diffuse large B-cell lymphoma by immunohistochemistry using a tissue microarray. Blood 103:275–282, 2004[Abstract/Free Full Text]
23. Harris NL. Mature B-cell neoplasms: introduction. In: Pathology and Genetics of Tumors of Haematopoietic and Lymphoid Tissues Jaffe ES, Harris NL, Stein H, Vardiman JW, eds. 121–126,IARC Press, Lyon, France. 2001
24. Ito M, Iida S, Inagaki H, Tsuboi K, Komatsu H, Yamaguchi M, Nakamura N, Suzuki R, Seto M, Nakamura S, Morishima Y, Ueda R. MUM1/IRF4 expression is an unfavorable prognostic factor in B-cell chronic lymphocytic leukemia (CLL)/small lymphocytic lymphoma (SLL). Jpn J Cancer Res 93:685–694, 2002[CrossRef][Web of Science]
25. Jacobs RM, Messick JB, Valli VE. Plasma cell neoplasia and multiple myeloma. In: Tumors in Domestic Animals Meuten DJ, ed. 4th ed., 161–165,Iowa State Press, Ames, IA. 2002
26. Jubala CM, Wojcieszyn JW, Valli VEO, Getzy DM, Fosmire SP, Coffey D, Bellgrau D, Modiano JF. CD20 expression in normal canine B cells and in canine non-Hodgkin lymphoma. Vet Pathol 42:468–476, 2005[Abstract/Free Full Text]
27. Kamijo T, Inagi K, Nakajima M, Motoori T, Tadokoro K, Nishiyama S. A case of extramedullary plasmacytoma of the larynx. Acta Otolaryngol Suppl 547:104–106, 2002[Medline]
28. Kremer M, Ott G, Nathrath M, Specht K, Stecker K, Alexiou C, Quintanilla-Martinez L, Fend F. Primary extramedullary plasmacytoma and multiple myeloma: phenotypic differences revealed by immunohistochemical analysis. J Pathol 205:92–101, 2005[CrossRef][Web of Science][Medline]
29. Kyriazidou A, Brown PJ, Lucke VM. An immunohistochemical study of canine extramedullary plasma cell tumors. J Comp Pathol 100:259–266, 1989[CrossRef][Web of Science][Medline]
30. Lester SJ, Mesfin GM. A solitary plasmacytoma in a dog with progression to a disseminated myeloma. Can Vet J 21:284–286, 1980[Web of Science][Medline]
31. Li W, Nagineni CN, Efiok B, Chepelinsky AB, Egwuagu CE. Interferon regulatory transcription factors are constitutively expressed and spatially regulated in the mouse lens. Dev Biol 210:44–55, 1999[CrossRef][Web of Science][Medline]
32. Linke RP, Geisel O, Mann K. Equine cutaneous amyloidosis derived from an immunoglobulin –light chain: immunohistochemical, immunochemical and chemical results. Biol Chem Hoppe-Seyler 372:835–843, 1991[Web of Science][Medline]
33. Lu R, Medina KL, Lancki DW, Singh H. IRF-4,8 orchestrate the pre-B-to-B transition in lymphocyte development. Genes Dev 17:1703–1708, 2003[Abstract/Free Full Text]
34. Mittrücker H-W, Matsuyama T, Grossman A, Kündig TM, Potter J, Shahinian A, Wakeham A, Patterson B, Ohashi PS, Mak TW. Requirement for the transcription factor LSIRF/IRF4 for mature B and T lymphocyte function. Science 275:540–543, 1997[Abstract/Free Full Text]
35. Morton LD, Barton CL, Elissalde GS, Wilson SR. Oral extramedullary plasmacytomas in two dogs. Vet Pathol 23:637–639, 1986[Web of Science][Medline]
36. Natkunam Y, Warnke RA, Montgomery K, Falini B, van den Rijn M. Analysis of MUM1/IRF4 protein expression using tissue microarrays and immunohistochemistry. Mod Pathol 14:686–694, 2001[CrossRef][Web of Science][Medline]
37. Platz SJ, Breuer W, Pfleghaar S, Minkus G, Hermanns W. Prognostic value of histopathological grading in canine extramedullary plasmacytomas. Vet Pathol 36:23–27, 1999[Abstract]
38. Rakich PM, Latimer KS, Weiss R, Steffens WL. Mucocutaneous plasmacytomas in dogs: 75 cases (1980-1987). J Am Vet Med Assoc 194:803–810, 1989[Web of Science][Medline]
39. Ramos-Vara JA, Beissenherz ME. Optimization of immunohistochemical methods using two different antigen retrieval methods on formalin-fixed, paraffin-embedded tissues: experience with 63 markers. J Vet Diagn Invest 12:307–311, 2000[Abstract/Free Full Text]
40. Ramos-Vara JA, Miller MA. Comparison of two polymer-based immunohistochemical detection systems: ENVISION+ and ImmPRESS. J Micros 224:135–139, 2006[CrossRef]
41. Ramos-Vara JA, Miller MA. Immunohistochemical detection of protein gene product 9.5 (PGP 9.5) in canine epitheliotropic T-cell lymphoma (mycosis fungoides). Vet Pathol 44:74–79, 2007[Abstract/Free Full Text]
42. Ramos-Vara JA, Miller MA, Pace LW, Linke RP, Common RS, Watson GL. Intestinal multinodular A-amyloid deposition associated with extramedullary plasmacytoma in three dogs: clinicopathological and immunohistochemical studies. J Comp Path 119:239–249, 1998[CrossRef][Web of Science][Medline]
43. Ramos-Vara JA, Takahashi M, Miller MA, Pace LW, Craft D, Common R, Watson GL. Intestinal extramedullary plasmacytoma associated with amyloid deposition in three dogs: an ultrastructural and immunoelectron microscopic study. Ultrastruct Pathol 22:393–400, 1998[Web of Science][Medline]
44. Ria R, Di Ianni M, Sportoletti P, Cimminiello M, Marcomigni L, Tabilio A. Recurrent primary plasmacytoma of the eyelid with rapid regional metastasis. Leuk Lymphoma 47:549–552, 2006[CrossRef][Web of Science][Medline]
45. Rowland PH, Valentine BA, Stebbins KE, Smith CA. Cutaneous plasmacytomas with amyloid in six dogs. Vet Pathol 28:125–130, 1991[Abstract]
46. Schrenzel MD, Naydan DK, Moore PF. Leukocyte differentiation antigens in canine cutaneous and oral plasmacytomas. Vet Dermatol 9:33–41, 1998[CrossRef][Web of Science]
47. Shapiro-Shelef M, Calame K. Plasma cell differentiation and multiple myeloma. Curr Opin Immunol 16:226–234, 2004[CrossRef][Web of Science][Medline]
48. Sundram U, Harvell JD, Rouse RV, Natkunam Y. Expression of the B-cell proliferation marker MUM1 by melanocytic lesions and comparison with S100, gp100 (HMB45), and melan A. Mod Pathol. 16:802–810, 2003
49. Sundram U, Kim Y, Mraz-Gernhard S, Hoppe R, Natkunam Y, Kohler S. Expression of the bcl-6 and MUM1/IRF4 proteins correlate with overall and disease-specific survival in patients with primary cutaneous large B-cell lymphoma: a tissue microarray study. J Cutan Pathol 32:227–234, 2005[CrossRef][Web of Science][Medline]
50. Suzuki S, Honma K, Matsuyama T, Suzuki K, Toriyama K, Akitoyo I, Yamamoto K, Suematsu T, Nakamura M, Yui K, Kumatori A. Critical roles of interferon regulatory factor 4 in CD11b^highCD8alpha-dendritic cell development. Proc Natl Acad Sci USA 101:8981–8986, 2004[Abstract/Free Full Text]
51. Taubenheim N, von Hornung M, Durandy A, Warnatz K, Corcoran L, Peter H-H, Eibel H. Defined blocks in terminal plasma cell differentiation of common variable immunodeficiency patients. J Immunol 175:5498–5503, 2005[Abstract/Free Full Text]
52. Tsuboi K, Iida S, Inagaki H, Kato M, Hayami Y, Hanamura I, Miura K, Harada S, Kikuchi M, Komatsu H, Banno S, Wakita A, Nakamura S, Eimoto T, Ueda R. MUM1/IRF4 expression as a frequent event in mature lymphoid malignancies. Leukemia 14:449–456, 2000[CrossRef][Web of Science][Medline]
53. Valli VE, Jacobs RM, Parodi AL, Vernau W, Moore PF. Histological classification of hematopoietic tumors of domestic animals. In: Histological Classification of Hematopoietic Tumors of Domestic Animals Valli VE, Jacobs RM, Parodi AL, Vernau W, Moore PF, eds. Air Forces Institute of Pathology, Washington, DC. 2002
54. Valli VE, Vernau W, de Lorimier LP, Gram PS, Moore PG. Canine indolent nodular lymphoma. Vet Pathol 43:241–256, 2006[Abstract/Free Full Text]
55. Vega F, Chang C-C, Medeiros LJ, Udden MM, Cho-Vega JH, Lau C-C, Finch CJ, Vilchez RA, McGregor D, Jorgenssen JL. Plasmablastic lymphomas and plasmablastic plasma cell myelomas have nearly identical immunophenotypic profiles. Mod Pathol 18:806–815, 2005[CrossRef][Web of Science][Medline]
56. Weedon D. Plasmacytomas and multiple myeloma. In: Skin Pathology Weedon D, ed. 2nd ed., 1062–1063,Churchill Livingstone, Edinburgh, UK. 2002
57. Wong KF, Chan JKC, Li LPK, Yau TK, Lee AWM. Primary cutaneous plasmacytoma: report of two cases and review of the literature. Am J Dermatopathol 16:392–397, 1994[Web of Science][Medline]

CiteULike    Complore    Connotea    Del.icio.us    Digg    Facebook    Reddit    Technorati    Twitter    What's this?

This article has been cited by other articles:

				J. A. Ramos-Vara, M. Kiupel, T. Baszler, L. Bliven, B. Brodersen, B. Chelack, S. Czub, F. D. Piero, S. Dial, E.J. Ehrhart, et al. Suggested guidelines for immunohistochemical techniques in veterinary diagnostic laboratories J Vet Diagn Invest, July 1, 2008; 20(4): 393 - 413. [Abstract] [Full Text] [PDF]

This Article Abstract Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Email this article to a friend Similar articles in this journal Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via HighWire Citing Articles via ISI Web of Science (1) Citing Articles via Google Scholar Google Scholar Articles by Ramos-Vara, J. A. Articles by Valli, V. E. O. Search for Related Content PubMed Articles by Ramos-Vara, J. A. Articles by Valli, V. E. O. Social Bookmarking                            What's this?