Non-Hodgkin Lymphoma Protocol applies to non-Hodgkin lymphoma involving any organ system except the gastrointestinal tract. Protocol revision date: January 2004 Procedures • Cytology (No Accompanying Checklist) • Biopsy • Resection of Lymph Node or Other Organ
Authors Carolyn Compton, MD, PhD
Department of Pathology, McGill University, Montreal, Quebec, Canada
Department of Pathology, UCLA School of Medicine, Los Angeles, California
For the Members of the Cancer Committee, College of American Pathologists Previous contributors: Nancy L. Harris, MD; Dennis W. Ross, MD, PhD; Annik van den Abbeele, MD; Judith Ferry, MD; Claire Fung, MD; Irene Kuter, MD; Peter Mauch, MD Non-Hodgkin Lymphoma • Hematologic System CAP Approved Surgical Pathology Cancer Case Summary (Checklist) Protocol revision date: January 2004 Applies to non-gastrointestinal, non-Hodgkin lymphoma only NON-HODGKIN LYMPHOMA: Biopsy/Resection
Patient name: Surgical pathology number: Note: Check 1 response unless otherwise indicated. MACROSCOPIC Specimen Type ___ Lymphadenectomy ___ Other (specify): ____________________________ ___ Not specified Tumor Site (check all that apply)
___ Lymph node(s), site not specified ___ Lymph node(s)
Specify site(s): _______________________________________
___________________________________________________
Specify site(s): _______________________________________
___________________________________________________
___ Not specified MICROSCOPIC Histologic Type (WHO Classification) ___ Histologic type cannot be assessed B-cell Lymphoma ___ B-cell lymphoma, subtype cannot be determined ___ Precursor B-lymphoblastic leukemia/lymphoma ___ Chronic lymphocytic leukemia/small lymphocytic lymphoma ___ B-cell prolymphocytic leukemia ___ Lymphoplasmacytic lymphoma ___ Splenic marginal zone lymphoma ___ Hairy cell leukemia ___ Plasma cell myeloma/ Plasmacytoma
* Data elements with asterisks are not required for accreditation purposes for
the Commission on Cancer. These elements may be clinically important,
but are not yet validated or regularly used in patient management.
Alternatively, the necessary data may not be available to the pathologist
at the time of pathologic assessment of this specimen.
CAP Approved Hematologic System • Non-Hodgkin Lymphoma
___ Extranodal marginal zone B-cell lymphoma of mucosa-associated lymphoid tissue
* Data elements with asterisks are not required for accreditation purposes for
the Commission on Cancer. These elements may be clinically important, but are not yet validated or regularly used in patient management. Alternatively, the necessary data may not be available to the pathologist at the time of pathologic assessment of this specimen.
Non-Hodgkin Lymphoma • Hematologic System CAP Approved
___ Nodal marginal zone B-cell lymphoma ___ Follicular lymphoma, grade 1 (0-5 centroblasts per HPF) ___ Follicular lymphoma, grade 2 (6-15 centroblasts per HPF) ___ Follicular lymphoma, grade 3 (greater than 15 centroblasts per HPF) ___ Follicular lymphoma, cutaneous follicle center sub-type ___ Follicular lymphoma, diffuse follicle center sub-type, grade 1
___ Follicular lymphoma, diffuse follicle center cell sub-type, grade 2
___ Mantle cell lymphoma ___ Diffuse large B-cell lymphoma ___ Mediastinal (thymic) large B-cell lymphoma ___ Intravascular large B-cell lymphoma ___ Primary effusion lymphoma ___ Burkitt lymphoma/leukemia ___ Lymphomatoid granulomatosis ___ Other (specify): ____________________________ T-cell Lymphoma ___ T-cell lymphoma, subtype cannot be determined ___ Precursor T-lymphoblastic leukemia/lymphoma ___ T-cell prolymphocytic leukemia ___ T-cell large granular lymphocytic leukemia ___ Aggressive NK-cell leukemia ___ Adult T-cell leukemia/lymphoma ___ Extranodal NK/T-cell lymphoma, nasal type ___ Enteropathy-type T-cell lymphoma ___ Hepatosplenic T-cell lymphoma ___ Subcutaneous panniculitis-like T-cell lymphoma ___ Mycosis fungoides / Sézary syndrome ___ Primary cutaneous anaplastic large cell lymphoma ___ Peripheral T-cell lymphoma, unspecified ___ Angioimmunoblastic T-cell lymphoma ___ Anaplastic large cell lymphoma ___ Lymphomatoid papulosis ___ Other (specify): ____________________________ Extent of Pathologically Examined Tumor (check all that apply) ___ Involvement of a single lymph node region
Specify site: ____________________________
___ Involvement of multiple lymph node regions
Specify: _______________________________
___ Splenic involvement ___ Liver involvement ___ Bone marrow involvement ___ Other organ involvement
Specify: ________________________________
* Data elements with asterisks are not required for accreditation purposes for
the Commission on Cancer. These elements may be clinically important,
but are not yet validated or regularly used in patient management.
Alternatively, the necessary data may not be available to the pathologist
at the time of pathologic assessment of this specimen.
CAP Approved Hematologic System • Non-Hodgkin Lymphoma
* Data elements with asterisks are not required for accreditation purposes for
the Commission on Cancer. These elements may be clinically important, but are not yet validated or regularly used in patient management. Alternatively, the necessary data may not be available to the pathologist at the time of pathologic assessment of this specimen.
Non-Hodgkin Lymphoma • Hematologic System CAP Approved Phenotyping ___ Performed, see separate report ___ Performed
Specify method and results: ______________________________
__________________________________________________
___ Not performed *Additional Pathologic Findings *Specify: _______________________________________ *Comment(s)
* Data elements with asterisks are not required for accreditation purposes for
the Commission on Cancer. These elements may be clinically important,
but are not yet validated or regularly used in patient management.
Alternatively, the necessary data may not be available to the pathologist
at the time of pathologic assessment of this specimen.
For Information Only Hematologic System • Non-Hodgkin Lymphoma Background Documentation Protocol revision date: January 2004 I. Cytologic Material A. Clinical Information
a. Name b. Patient identification number c. Age (birth date) (Note A) d. Sex (Note B)
2. Responsible physician(s) 3. Date of procedure 4. Other clinical information
a. Relevant history (eg, duration of lymphadenopathy or other mass; previous
diagnosis and treatment for lymphoma, Hodgkin lymphoma, or other malignancy; immunosuppression; AIDS; bone marrow or solid organ transplantation)
b. Relevant findings (eg, distribution of lymphadenopathy, signs and
symptoms, imaging studies, serum lactate dehydrogenase [LDH] level) (Note C)
c. Clinical diagnosis d. Clinical stage, if known e. Specific procedure (fine-needle aspiration [FNA], tap of effusion, other) f. Operative findings g. Anatomic site(s) of specimen(s) (Note D) B. Macroscopic Examination
a. Unfixed/fixed (specify fixative) b. Number of slides received, if appropriate c. Quantity and appearance of fluid specimen, if appropriate d. Other (eg, cytologic preparation from tissue) e. Results of intraprocedural consultation
2. Material submitted for microscopic evaluation (eg, FNA, cytospin of fluid, other) 3. Special studies, specify (eg, flow cytometry for immunophenotyping,
cytochemistry, immunohistochemistry, cytogenetic analysis)
C. Microscopic Evaluation
1. Adequacy of specimen (if unsatisfactory for evaluation, specify reason) 2. Lymphoma, if present
a. Histologic type, if possible (Note E) b. Other characteristics (eg, necrosis)
3. Additional pathologic findings, if present 4. Results /status of special studies (specify) 5. Comments
a. Correlation with intraprocedural consultation, as appropriate b. Correlation with other specimens, as appropriate c. Correlation with clinical information, as appropriate
Non-Hodgkin Lymphoma • Hematologic System For Information Only II. Biopsy A. Clinical Information
a. Name b. Patient identification number c. Age (birth date) (Note A) d. Sex (Note B)
2. Responsible physician(s) 3. Date of procedure 4. Other clinical information
a. Relevant history (eg, duration of lymphadenopathy or other mass; previous
diagnosis and treatment for lymphoma, Hodgkin lymphoma, or other malignancy; immunosuppression; AIDS; bone marrow or solid organ transplantation)
b. Relevant findings (eg, distribution of lymphadenopathy, signs and
symptoms, imaging studies, serum LDH level) (Note C)
c. Clinical diagnosis d. Clinical stage, if known e. Specific procedure (eg, lymph node biopsy, liver biopsy) f. Operative findings g. Anatomic site(s) of specimen(s) (Note D) B. Macroscopic Examination
a. Unfixed/fixed (specify fixative) (Note: When appropriate, fresh sterile tissue
should be sent for culture, and fresh frozen tissue should be saved, if possible, for immunophenotyping and molecular genetic studies)
b. Number of pieces c. Largest dimension of each piece d. Results of intraoperative consultation
2. Submit nonfrozen tissue for microscopic evaluation 3. Special studies, specify (eg, flow cytometry for immunophenotyping,
cytochemistry, immunohistochemistry, cytogenetic analysis) (Note F) C. Microscopic Evaluation
a. Histologic type (Note E) b. Other characteristics (eg, necrosis)
2. Additional pathologic findings, if present 3. Results/status of special studies 4. Comments
a. Correlation with intraoperative consultation, as appropriate b. Correlation with other specimens, as appropriate c. Correlation with clinical information, as appropriate
III. Resection of Lymph Node or Other Organ A. Clinical Information
a. Name b. Patient identification number c. Age (birth date) (Note A) For Information Only Hematologic System • Non-Hodgkin Lymphoma
d. Sex (Note B)
2. Responsible physician(s) 3. Date of procedure 4. Other clinical information
a. Relevant history (eg, duration of lymphadenopathy or other mass; previous
diagnosis and treatment for lymphoma, Hodgkin disease, or other malignancy; immunosuppression; AIDS; bone marrow or solid organ transplantation)
b. Relevant findings (eg, distribution of lymphadenopathy, signs and
symptoms, imaging studies, serum LDH level) (Note C)
c. Clinical diagnosis d. Clinical stage, if known e. Specific procedure (eg, lymph node excision, splenectomy, other) f. Operative findings g. Anatomic site(s) of specimen(s) (Note D) B. Macroscopic Examination
a. Organ(s)/tissue(s) (Note D) b. Unfixed/fixed (specify fixative) (Note: When appropriate, fresh sterile tissue
should be sent for culture and fresh frozen tissue should be saved for immunophenotyping and molecular genetic studies)
c. Number of pieces d. Dimensions e. Orientation of specimen, if indicated by surgeon f. Results of intraoperative consultation
a. Number of lesions (Note G) b. Location (Note G) c. Configuration d. Dimensions e. Descriptive characteristics (eg, color, consistency) f. Direct extension to other organ(s) or structure(s) (Note H) g. Noncontiguous tumor involvement of other organ(s) or structure(s) (Note G)
3. Other lesions 4. Tissues submitted for microscopic evaluation
a. Lymphoma, representative sections b. Other specific nodes, when marked by surgeon c. Other lesions d. Section(s) of tissue uninvolved by tumor e. Other tissue(s)/organ(s)
5. Special studies, specify (eg, flow cytometry for immunophenotyping,
cytochemistry, immunohistochemistry, cytogenetic analysis) (Note F)
a. Histologic type (Note E) b. Direct extension to other organ(s) or structure(s)
2. Additional pathologic findings, if present (eg, reactive follicular hyperplasia) 3. Other tissues submitted (if distant involvement by lymphoma, specify site)
Non-Hodgkin Lymphoma • Hematologic System For Information Only
4. Results/status of special studies (specify) 5. Comments
a. Correlation with intraoperative consultation, as appropriate b. Correlation with other specimens, as appropriate c. Correlation with clinical information, as appropriate
Explanatory Notes A. Patient Age Age is a risk factor independently associated with survival in non-Hodgkin lymphoma (NHL). Age above 60 years has been shown to be associated with decreased survival compared to age 60 or less.1-4 In some series of patients with low grade NHL, age greater than 40 has been associated with decreased survival.5 Across all grades and stages of NHL, a decreased ability of patients greater than 60 years of age to tolerate treatment may be the major effect of age.3 However, even among patients treated equivalently for low stage disease (ie, stage I and II, see below), older patients are at greater risk for relapse than younger patients.3,6-16 B. Sex Across all grades and stages of NHL, male sex has been shown to correlate with other adverse prognostic factors such as histologic type, stage, and symptoms (see below). However, it has also been demonstrated to have independent adverse prognostic significance in patients with low grade NHL.5,14,17 C. Clinical Findings Although not always provided to the pathologist by the physician submitting the specimen, certain specific clinical findings are known to be of prognostic value in NHL (across all stages). In particular, systemic symptoms of fever (greater than 38.5°C), unexplained weight loss (more than 10% body weight) in the 6 months before diagnosis, and drenching night sweats are used to define 2 categories for each stage of NHL: A (symptoms absent), and B (symptoms present). The presence of B symptoms is known to correlate with extent of disease (stage and tumor bulk), but symptoms also have been shown to have prognostic significance for cause-specific survival that is independent of stage.3,4,6,13,18,19 Poor patient “performance status” has also been shown by several multivariate analyses to have independent adverse prognostic significance.1,6,10,17 Performance status refers to the overall activity level of the patient ranging from fully active to completely bed-ridden, and a poor performance status is usually defined as any degree of activity less than fully active or fully ambulatory (ie, bed-ridden for varying proportions of time).1,2 Elevated serum lactate dehydrogenase (LDH) level is an adverse prognostic factor that correlates with tumor burden (stage and bulk).3 It has also been shown to have independent prognostic significance in both early and late stage NHL in many studies.8,12,16,20-25 Tumor bulk, usually defined by clinical and/or imaging studies, is a predictive factor in various settings.3 A tumor greater than 5 to 10 cm in diameter is associated with higher For Information Only Hematologic System • Non-Hodgkin Lymphoma
rates of relapse of stage I and II NHL treated with radiotherapy.13 A tumor greater than 10 cm in diameter is associated with poor outcome in patients with stage III and IV NHL treated with chemotherapy.3 Other definitions of bulky disease associated with poor outcome in stage II to IV NHL include a large mediastinal mass (greater than one-third of chest diameter), a palpable abdominal mass, and a combination of para-aortic and pelvic node involvement.3,4,7,13,16,17,23,26 D. Anatomic Sites The anatomic sites that constitute the major structures of the lymphatic system include groups and chains of lymph nodes, the spleen, the thymus, Waldeyer’s ring (a circular band of lymphoid tissue that surrounds the oropharynx consisting of the palatine, lingual, and pharyngeal tonsils), the vermiform appendix, and the Peyer’s patches of the ileum. Minor sites of lymphoid tissue include the bone marrow, liver, skin, lung, pleura, and gonads. Involvement of extranodal sites is more common in NHL than in Hodgkin lymphoma. E. Histologic Type
The protocol recommends the World Health Organization (WHO) Classification of Lymphoid Neoplasms, which is shown below.27,28 This classification encompasses both nodal and extranodal lymphomas and outlines the immunobiologic features of the defined entities that aid in the diagnosis. The prognostic information necessary to determine treatment of lymphoma is, in general, provided by the histologic type.
WHO Classification of Lymphoid Neoplasms
B-cell Neoplasms Precursor B-cell neoplasms
Precursor B-lymphoblastic lymphoma/leukemia
Chronic lymphocytic leukemia/small lymphocytic lymphoma
Lymphoplasmacytic lymphoma / Waldenström macroglobulinemia
Extranodal marginal zone B-cell lymphoma of mucosa-associated lymphoid
Grade 1: 0 to 5 centroblasts per high power field#
Grade 2: 6 to 15 centroblasts per high power field#
Grade 3: greater than 15 centroblasts per high power field#
Non-Hodgkin Lymphoma • Hematologic System For Information Only
Grade 3b: centroblasts form solid sheets with no residual
Follicular and diffuse: 25% to 75% follicular
Focally follicular: less than 25% follicular
Grade 1: 0 to 5 centroblasts per high power field#
Grade 2: 6 to 15 centroblasts per high power field#
Variants: Blastoid (classic or pleomorphic), others
Burkitt lymphoma with plasmacytoid differentiation
B-cell proliferations of uncertain malignant potential
Post-transplant lymphoproliferative disorder, polymorphic
# WHO guideline27 for high powered field (HPF) = high powered field of 0.159mm2 (40X objective, 18mm field of view ocular; count 10 HPF and divide by 10). If using a 10mm field of view ocular, count 8 HPF and divide by 10, or count 10 HPF and divide by 12 to get the number of centroblasts/0.159mm2 HPF. If using a 22-mm field of view ocular, count 7 HPF and divide by 10, or count 10 HPF and divide by 15 to get the number of centroblasts/0.159mm2 HPF. T-cell Neoplasms Precursor T-cell neoplasms
Precursor T lymphoblastic lymphoma/leukemia
Variants: small cell, cerebriform cell (Sézary cell-like)
For Information Only Hematologic System • Non-Hodgkin Lymphoma
Extranodal NK/T-cell lymphoma, nasal type
Variants: gamma-delta T-cell lymphoma in other anatomic sites
Subcutaneous panniculitic-like T-cell lymphoma
Mycosis fungoides (MF) and Sézary syndrome
Primary cutaneous anaplastic large cell lymphoma (C-ALCL)
T-cell proliferation of uncertain malignant potential
Immunophenotypes and Genetics26-29 Precursor B lymphoblastic leukemia/lymphoma: Slg-, cytoplasmic µ chain 30%, CD19+, CD20-/+, CD22+, CD79a+, TdT+, HLA-DR+, CD10+/-, CD34+/-, CD13-/+, CD33-/+, IgH gene rearrangement +/-, IgL gene rearrangement -/+, TCR gene rearrangement -/+, variable cytogenetic abnormalities B-cell chronic lymphocytic leukemia (B-CLL): Faint SIgM+, SIgD+/-, CIg-/+, panB+ (CD19+, CD20+), CD5+, CD10-, CD23+, CD43+, CD11c-/+; IgH and IgL gene rearrangements; trisomy 12-/+; 13q abnormalities-/+ Lymphoplasmacytic lymphoma: SIgM+, SIgD-/+, CIg+, PanB+, CD5-, CD10-, CD43+/-, CD25-/+; IgH and IgL gene rearrangements Splenic marginal zone lymphoma: SIgM+, SIgD+, CD20+, CD79a+, CD5-, CD10-, CD23-, CD43-, nuclear cyclin D1-, CD103-, allelic loss at 7q21-32 (40% of cases) Hairy cell leukemia: SIg+ (IgM, IgD, IgG, or IgA), PanB+, CD79a+, CD79b-, DBA.44+, CD5-, CD10-, CD23-, CD11c+, CD25+, FMC7+, CD103+ (mucosal lymphocyte antigen as detected by B-ly7), tartrate resistant acid phosphatase (TRAP)+; IgH and IgL gene rearrangements Plasma cell myeloma: CIg+ (IgG, IgA, rare IgD, IgM, or IgE or light chain only), PanB-, (CD19-, CD20-, CD22-), CD79a+/-, CD45-/+, HLA-DR-/+, CD38+, CD56+/-, EMA-/+, CD43+/-; IgH and IgL gene rearrangements; deletions most commonly 13q, and occasional translocations, in particular t(11;14)(q13;q32) Non-Hodgkin Lymphoma • Hematologic System For Information Only
Extranodal marginal zone B-cell lymphoma of MALT ( MALT lymphoma): SIg+ (IgM or IgA or IgG), SIgD-, CIg-/+, PanB+, CD5-, CD10-, CD23-, CD43-/+; IgH and IgL gene rearrangements, bcl-1 and bcl-2 germline, trisomy 3 or t(11;18)(q21;q21) may be seen Nodal marginal zone B-cell lymphoma : SIgM+, SIgD-, CIg-/+, PanB+, CD5-, CD10-, CD23-, CD43-/+; IgH and IgL gene rearrangements, bcl-1 and bcl-2 germline Follicular lymphoma: SIg+ (usually IgM +/- IgD, IgG, IgA), PanB+, CD10+/-, CD5-, CD23-/+, CD43-, CD11c-, CD25-; overexpression of BCL-2+ (useful to distinguish from reactive follicles); BCL6+ IgH and IgL gene rearrangements, t(14;18) with rearranged BCL-2 gene in 70-95% of cases Mantle cell lymphoma: SIgM+, SIgD+, lambda>kappa, PanB+, CD5+, CD10-/+, CD23-, CD43+, CD11c-, CD25-; IgH and IgL gene rearrangements, t(11;14); bcl-1 gene rearrangements (CCND1/cyclinD1/PRAD1) common Diffuse large B-cell lymphoma: SIg+/-, CIg-/+, PanB+, CD45+/-, CD5-/+, CD10-/+ (weak); IgH and IgL gene rearrangements; bcl-2 gene rearranged in 30% of cases, bcl-6/LAZ3 gene (chromosome 3q27) rearranged in 30% of cases, c-myc gene rearrangement uncommon Mediastinal (thymic) large B-cell lymphoma: SIg-/+, PanB+, (especially CD20, CD79a), CD45+/-, CD15-, CD30-/+ (weak); IgH and IgL gene rearrangements Burkitt lymphoma: SIgM+, PanB+, CD5-, CD10+, CD23-; IgH and IgL gene rearrangements, t(8;14) and variants t(2;8) and t(8;22); rearranged c-myc gene. EBV common (95%) in endemic cases and infrequent (15-20%) in sporadic cases, intermediate incidence (30-40%) in HIV-positive cases Atypical Burkitt/ Burkitt-like lymphoma: SIg+/- (IgM or IgG), CIg-/+, PanB+, CD5-, CD10-/+; IgH and IgL gene rearrangements, infrequent rearrangement of c-myc gene, bcl-2 gene rearranged in 30% of cases Precursor T-lymphoblastic lymphoma/leukemia: TdT+, CD7+, CD3+/-, variable expression of other PanT antigens, CD1a+/-, often CD4 and CD8 double positive or negative, Ig-, PanB-; variable rearrangement of TCR genes; IgH gene rearrangement -/+, most common chromosomal abnormalities involve 14q11-14 or 7q35; variable cytogenetic abnormalities reported T-cell prolymphocytic leukemia: TdT-, PanT+, (CD2, CD3, CD5, CD7) CD25-, CD4+/CD8->CD4+/CD8+>CD4-/CD8-; TCR gene rearrangements, 75% of cases show inv 14(q11;q32) T-cell large granular lymphocytic leukemia, T-cell type: TdT-, PanT+ (CD2, CD3+, CD5+/-, CD7-), TCR+, CD4-, CD8+, CD16+, CD56-, CD57+, CD25-; most cases show clonal rearrangements of TCR genes T- cell large granular lymphocytic leukemia, NK-cell type: TdT-, CD2+, CD3-, TCR-, CD4-, CD8+/-, CD16+/-, CD56+/-, CD57+/-, CD25-; TCR and Ig genes are germline
For Information Only Hematologic System • Non-Hodgkin Lymphoma
Adult T-cell lymphoma/leukemia (HTLV1+): TdT-, PanT+ (CD2+, CD3+, CD5+, CD7-) CD4+, CD8-, CD25+; TCR gene rearrangements, clonally integrated HTLV1 Extranodal NK/T-cell lymphoma, nasal type: TdT-, CD2+, CD5-/+, CD7-/+, CD3-/+, may be CD4+ or CD8+, CD56+/-; usually no rearranged TCR or Ig genes; often EBV positive Enteropathy-type T-cell lymphoma: TdT-, CD3+, CD7+, CD4-, CD8+/-, CD103+ (mucosal lymphocyte antigen, such as detection by HML-1) (see gastrointestinal lymphoma protocol) Hepatosplenic T-cell lymphoma : CD2+, CD3+, TCR gamma-delta+, TCRab-, CD5-, CD7+, CD4-, CD8-/+, CD56+/-, CD25-; TCR- gene rearrangements, variable TCR- gene rearrangements Mycosis fungoides/Sézary syndrome: TdT-, PanT+ (CD2+, CD3+, CD5+, CD7-/+), most cases CD4+/CD8-, CD25-/+; TCR gene rearrangements Angioimmunoblastic T-cell lymphoma: TdT-, PanT+ (often with variable loss of some PanT antigens), usually CD4+; TCR gene rearrangements in 75%; IgH gene rearrangements in 10%, EBV often positive, but usually only in isolated neoplastic or reactive cells Peripheral T-cell lymphomas, unspecified: TdT-, PanT variable (CD2+/-, CD3+/-, CD5+/-, CD7-/+), most cases CD4+, some cases CD8+, CD4-/CD8-, or CD4+/CD8+; TCR gene rearrangements usual Anaplastic large cell lymphoma: TdT-, CD30+, EMA+/-, PanT-/+, CD45+/-, CD25+/-, CD15-/+, CD68-, lysozyme-, BNH9+/-; primary cutaneous form is EMA- and cutaneous lymphocyte antigen+; TCR gene rearrangements > germline, 12-50% of adult cases show t(2;5) resulting in a fusion on NPM gene (5q35) with ALK gene (2q23) F. Special Studies: Specimen Handling Specimens for the diagnosis of lymphoma require special handling in order to optimize the histologic diagnosis and to prepare the tissue for performance of molecular and other special studies. The guidelines detailed below are suggested for specimen handling in cases of suspected lymphoma. • Tissue should be received fresh. Unsectioned lymph nodes should not be immersed
• The fresh specimen size, color and consistency should be recorded, as should the
presence or absence of any visible nodularity, hemorrhage, or necrosis after serial sectioning at 2-mm intervals perpendicular to the long axis of a lymph node.
• Touch imprints may be made from the freshly cut surface, and the imprints fixed in
• For cytogenetic studies or culture of microorganisms: submit a portion of the node
• Fixation (record fixative[s] used for individual slices of the specimen):
• B5 produces superior cytologic detail but is not suitable for DNA extraction and
may impair some immunostains (eg, CD30).
Non-Hodgkin Lymphoma • Hematologic System For Information Only
• Over-fixation (ie, more than 24 hours in formalin, more than 4 hours in B5)
• Snap-frozen tissue is optimal for some immunostains and for DNA and RNA
extractions. • Cover tissue samples (cut to approximately 1x1x0.3 cm) in OCT.
• Immerse in dry ice/isopentane slush or liquid nitrogen.
G. Stage In general, the TNM classification has not been used for staging of lymphomas because the site of origin of the tumor is often unclear and there is no way to differentiate among T, N, and M. Thus, a special staging system (Ann Arbor System) is used for both Hodgkin lymphoma and NHL. The Ann Arbor classification for lymphomas has been applied to NHL by the American Joint Committee (AJCC) on Cancer and the International Union Against Cancer (UICC) (see below).30,31 For multiple myeloma, the Durie-Salmon staging system is recommended by the AJCC. Both staging systems are shown below. Pathologic staging depends on biopsy or resection of one or more regional lymph nodes, splenectomy, wedge liver biopsy, bone marrow biopsy, and biopsy of multiple lymph nodes on both sides of the diaphragm to assess distribution of disease. Clinical staging generally involves a combination of clinical, radiologic, and surgical procedures and includes medical history, physical examination, laboratory tests (eg, complete blood examination, and blood chemistry studies), imaging studies (eg, computed tomography [CAT] scans, magnetic resonance imaging [MRI] studies, and nuclear medicine studies), biopsy to determine diagnosis, extent of disease, and histologic type of tumor (initial diagnosis is almost always made on biopsy), and often bone marrow biopsy. Most commonly, staging of NHL is clinical rather than pathologic. There is almost universal agreement that the stage of NHL is prognostically significant.1-3,6,8,13,17,21 AJCC/UICC Staging for Non-Hodgkin Lymphomas30,31 Stage I
Involvement of a single lymph node region (I) or localized involvement of a single extralymphatic organ or site in the absence of any lymph node involvement (IE)#, ##
Involvement of 2 or more lymph node regions on the same side of the diaphragm (II), or localized involvement of a single extralymphatic organ or site in association with regional lymph node involvement with or without involvement of other lymph node regions on the same side of the diaphragm (IIE) ##,###
Involvement of lymph node regions on both sides of the diaphragm (III), which also may be accompanied by extralymphatic extension in association with adjacent lymph node involvement (IIIE) or by involvement of the spleen (IIIS) or both (IIIE+S) ##,###, ^
Diffuse or disseminated involvement of 1 or more extralymphatic organs, with or without associated lymph node involvement; or isolated extralymphatic organ involvement in the absence of adjacent regional lymph node involvement, but in conjunction with disease in distant
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site(s). Any involvement of the liver or bone marrow, or nodular involvement of the lung(s). ##,###,^
# Multifocal involvement of a single extralymphatic organ is classified as stage IE and not stage IV. ## For all stages, tumor bulk greater than 10 to 15 cm is an unfavorable prognostic factor.3 ### The number of lymph node regions involved may be indicated by a subscript: eg, II3. For stages II to IV, involvement of more than 2 sites is an unfavorable prognostic factor.3 ^ For stages III to IV, a large mediastinal mass is an unfavorable prognostic factor.3
AJCC/UICC Staging for Plasma Cell Myeloma30,31 Stage I
Normal bone x-rays or a solitary bone lesion
One or more of the following are included:
Disease fitting neither stage I nor stage III
Note: Patients are further classified as (A) serum creatinine less than 2.0 mg/dL, or (B) serum creatinine 2.0 mg/dL or greater. The median survival for stage IA disease is about 5 years, and that for stage IIIB disease is 15 months.30 H. Direct Spread into Adjacent Tissues or Organs Direct spread of a lymphoma into adjacent tissues or organs does not influence classification of stage. References 1. Shipp MA, Harrington DP, Anderson JR, et al. A predictive model for aggressive
non-Hodgkin lymphoma. N Engl J Med. 1993;329:987-994.
2. Shipp MA. Prognostic factors in aggressive non-Hodgkin lymphoma. Blood.
3. Crump M, Gospodarowicz MK. Non-Hodgkin malignant lymphoma. In:
Gospodarowicz MK, Henson DE, Hutter RVP, O’Sullivan B, Sobin LH, Wittekind C, eds. Prognostic Factors in Cancer. New York, NY: Wiley-Liss; 2001:689-703.
Non-Hodgkin Lymphoma • Hematologic System For Information Only
4. Gospodarowicz MK, Bush RS, Brown TC, et al. Prognostic factors in nodular
lymphomas: a multivariate analysis based on the Princess Margaret experience. Int J Radiat Oncol Biol Phys. 1984;10:489-497.
5. Dana BW, Dahlberg S, Nathwani BN, et al. Long-term follow-up of patients with
low-grade malignant lymphomas treated with doxorubicin-based chemotherapy or chemoimmunotherapy. J Clin Oncol. 1993;11:644-651.
6. Hayward RL, Leonard RC, Prescott RJ, et al. A critical analysis of prognostic
factors for survival in intermediate and high grade non-Hodgkin lymphoma: Scotland and Newcastle Lymphoma Group Therapy Working Party. Br J Cancer. 1991;63:945-952.
7. Kaminski MS, Coleman CN, Colby TV, et al. Factors predicting survival in adults
with stage I and II large-cell lymphoma treated with primary radiation therapy. Ann Intern Med. 1986;104:747-56.
8. Lindh J, Lenner P, Osterman B, et al. Prognostic significance of serum lactic
dehydrogenase levels and fraction of S-phase cells in non-Hodgkin lymphomas. Eur J Hematol. 1993;50:258-263.
9. O’Reilly SE, Hoskins P, Klimo P, et al. MACOP-B and VACOP-B in diffuse large
lymphomas and MOPP/ABV in Hodgkin disease. Ann Oncol. 1991;1:17-23.
10. Shimoyama M, Ota K, Kitutchi M, et al. Major prognostic factors of adult factors of
adult patients with advanced B-cell lymphoma treated with vincristine, cyclophosphamide, prednisone and doxorubicin (VEPA) or VEPA plus methotrexate (VEPA-M). Jpn J Clin Oncol. 1988;18:113-124.
11. Soubeyran P, Eghbali H, Bonichon, et al. Localized follicular lymphomas:
prognosis and survival of stage I and II in a retrospective series of 103 patients. Radiother Oncol. 1988;13:91-98.
12. Stein RS, Greer JP, Cousar JB, et al. Malignant lymphomas of follicular centre cell
origin in man, VII: prognostic features in small cleaved lymphoma. Hematol Oncol. 1989;7:381-391.
13. Sutcliffe SB, Gospodarowicz MK, Bush RS, et al. Role of radiation therapy in
localized non-Hodgkin lymphoma. Radiother Oncol. 1985;4:211-223.
14. Taylor RE, Allan SG, McIntyre MA, et al. Low grade stage I and II non-Hodgkin
lymphoma: results of treatment and relapse pattern following therapy. Clin Radiol. 1988;39:287-290.
15. Velasquez WS, Fuller LM, Jagannath S, et al. Stages I and II diffuse large cell
lymphomas: prognostic factors and long-term results with CHOP-bleo and radiotherapy. Blood. 1991;77:942-947.
16. Velasquez WS, Jagannath S, Tucker TS, et al. Risk classification as the basis for
clinical staging of diffuse large-cell lymphoma derived from 10-year survival data. Blood. 1989;74:551-557.
17. Steward WP, Crowther D, McWilliam LJ, et al. Maintenance chlorambucil after
CVP in the management of advanced stage, low grade histologic type non-Hodgkin lymphoma: a randomized prospective study with assessment of prognostic factors. Cancer. 1988;61:441-447.
18. Hoskins PJ, Ng V, Spinelli JJ, et al. Prognostic variables in patients with diffuse
large-cell lymphoma treated with MACOP-B. J Clin Oncol. 1991;9:220-226.
19. O’Reilly SE, Hoskins P, Klimo P, et al. Long-term follow-up of pro-MACE-CytoBOM
in non-Hodgkin lymphoma. Ann Oncol. 1991;1:33-35.
For Information Only Hematologic System • Non-Hodgkin Lymphoma
20. Bastion Y, Berger F, Bryon PA, et al. Follicular lymphomas: assessment of
prognostic factors in 127 patients followed for 10 years. Ann Oncol. 1991;(suppl 2):123-129.
21. Cowan RA, Jones M, Harris M, et al. Prognostic factors in high and intermediate
grade non-Hodgkin lymphoma. Br J Cancer. 1989;59:276-282.
22. Kwak LW, Halpern J, Olshen RA, et al. Prognostic significance of actual dose
intensity in diffuse large-cell lymphoma: results of a tree-structured survival analysis. J Clin Oncol. 1990;8:963-977.
23. Prestidge BR, Horning SJ, Hoppe RT. Combined modality therapy for stage I-II
large cell lymphoma. Int J Radiat Oncol Biol Phys. 1988;15:633-639.
24. Straus DJ, Wong G, Yahalom J, et al. Diffuse large cell lymphoma: prognostic
factors with treatment. Leukemia. 1991;1:32-37.
25. Vitolo U, Bertini M, Brusamolina E, et al. MACOP-B treatment in diffuse large cell
lymphoma: identification of prognostic groups in an Italian multicenter study. J Clin Oncol. 1992;10:219-227.
26. Jaffe ES, Harris NL, Stein H, Vardiman JW, eds. World Health Organization Classification of Tumours. Pathology and Genetics. Tumours of Haematopoietic and Lymphoid Tissues. Lyon (France): IARC Press; 2001.
27. Stein H, Delsol G, Pileri S, et al. WHO histological classification of Hodgkin
lymphoma. In: Jaffe ES, Harris NL, Stein H, Vardiman JW, eds. World Health Organization Classification of Tumours. Pathology and Genetics. Tumours of Haematopoietic and Lymphoid Tissues. Lyon (France): IARC Press; 2001.
28. Harris NL, Jaffe ES, Stein H, et al. A revised European-American classification of
lymphoid neoplasms: a proposal from the International Lymphoma Study Group. Blood. 1994;84:1361-1392.
29. Chan JKC, Banks PM, Cleary ML, et al. A revised European-American
classification of lymphoid neoplasms: a proposal from the International Lymphoma Study Group: a summary version. Am J Clin Pathol. 1995;103:543-560.
30. Greene FL, Page DL, Fleming ID, et al, eds. AJCC Cancer Staging Manual. 6th ed.
31. Sobin LH, Wittekind C, eds. UICC TNM Classification of Malignant Tumours. 6th
Bibliography Coiffier B, Gisselbrecht C, Vose JM, et al. Prognostic factors in aggressive malignant
lymphomas: description and validation of a prognostic index that could identify patients requiring a more intensive therapy. J Clin Oncol. 1991;9:211-219.
Collins RD. Lymph node examination: what is an adequate work-up? Arch Pathol Lab
Cousar JB. Surgical pathology examination of lymph nodes. Am J Clin Pathol.
Gordon LI, Andersen J, Colgan J, et al. Advanced non-Hodgkin lymphoma: analysis of
prognostic factors by the International Index and by lactic dehydrogenase in an intergroup study. Cancer. 1995;75:865-873.
Kramer MHH, Hermans J, Parker J, et al. Clinical significance of bcl2 and p53 protein
expression in diffuse large B-cell lymphoma: a population-based study. J Clin Oncol. 1996;14:2131-2138.
Liang R, Todd D, Ho FC: Aggressive non-Hodgkin lymphoma: T-cell versus B-cell.
Non-Hodgkin Lymphoma • Hematologic System For Information Only
Osterman B, Cavallin-Stahl E, Hagberg H, et al. High-grade non-Hodgkin lymphoma
stage I: a retrospective study of treatment, outcome, and prognostic factors in 213 patients. Acta Oncol. 1996;35:171-177.
Stauder R, Eisterer W, Thaler J, et al. CD44 variant isoforms in non-Hodgkin’s
lymphoma: a new independent prognostic factor. Blood. 1995;85:2885-2889.
DISPONIBLES DANS VOTRE SALON LE REFLET CHALONNESPROGRAMME CHEVEUX FINS ET SANS VOLUMEGalbe et volume aérien…Les cheveux fins manquent souvent de volume et de tonus. Difficiles à coiffer, ils n’ont aucune tenue. Vos cheveux ont besoin d’être gainés et hydratés. Ils retrouvent ainsi peu à peu la texture qui donne à votre coiffure un volume aérien, un galbe merveilleux, de la racine au
Two respondents to the survey noted the many opportunities for workers in met-ropolitan areas to engage in feminist activism (such as forums, meetings andactivities like “Reclaim the Night” marches) in contrast to their own contextswhere a public show of feminist solidarity and shared purpose could potentiallybe met with community contempt. Workers also spoke of the added complexitiesof needin