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Featured researches published by David W. Bahler.


American Journal of Pathology | 2000

Histological and Immunoglobulin VH Gene Analysis of Interfollicular Small Lymphocytic Lymphoma Provides Evidence for Two Types

David W. Bahler; Nadine S. Aguilera; Carolyn C. Chen; Susan L. Abbondanzo; Steven H. Swerdlow

Interfollicular small lymphocytic lymphoma (I-SLL) has not been well characterized and its relationship to small lymphocytic lymphoma (SLL) or chronic lymphocytic leukemia (CLL) is uncertain. Moreover, two different proliferation center growth patterns have been described with respect to reactive germinal centers. In this study, we evaluate the histological and immunophenotypic features of 13 cases of I-SLL and immunoglobulin heavy chain variable (VH) gene sequences from 10 cases. Immunophenotypic analyses indicate that cases showing either growth pattern have the same CD5-positive B cell phenotype typical of SLL or CLL. Sequence analysis revealed the use of VH, D, and J gene segments often found in CLL, although there may be more frequent use of J6. Similar to recent studies of CLL, there were approximately equal numbers of cases with either mutated or unmutated VH genes without evidence of ongoing mutation, consistent with I-SLL having either a naïve or memory B cell origin. Interestingly, the mutational status of the I-SLL VH genes seemed to correlate with the two different histological growth patterns. These studies support the proposal that I-SLL represents SLL/CLL and suggest the recently proposed two types of CLL originating from either memory or naïve B cells may have different histological patterns of growth in lymph nodes that show architectural preservation.


Modern Pathology | 2009

Use of similar immunoglobulin VH gene segments by MALT lymphomas of the ocular adnexa

David W. Bahler; Philippe Szankasi; Sucheta Kulkarni; Raymond R. Tubbs; James R. Cook; Steven H. Swerdlow

Extranodal marginal zone lymphomas of mucosa-associated lymphoid tissue type (MALT lymphomas) develop from acquired reactive infiltrates directed against external or autoantigens. Although some European cases of ocular adnexal MALT lymphoma have been associated with Chlamydia psittaci infections, C. psittaci has not been detected in large studies of US-based cases. To evaluate whether the growth of US-based ocular adnexal MALT lymphomas may be promoted by a similar antigen, we identified and analyzed the expressed immunoglobulin VH genes in 10 cases. Interestingly, the VH genes in two cases used the same VH1 family V1-2 gene segment, and three cases used the same VH4 family V4-34 gene segment. The other five cases all used different gene segments V4-31, V5-51, V3-23, V3-30, and V3-7. All of the VH genes were mutated from germ line, with percent homologies ranging between 96.9 and 89.0%. The distribution of replacement and silent mutations within the VH genes was nonrandom consistent with the maintenance of immunoglobulin function and also strongly suggestive of antigen selection in the six VH genes with highest mutation loads. The CDR3 sequences in two of three VH-34 cases were the same size (15 amino acids) and had similar sizes in the two VH1-2 cases (18 and 16 amino acids). In conclusion, US-based MALT lymphomas of the ocular adnexa preferentially express a limited set of VH gene segments not frequently used by other MALT lymphomas and consistent with some recognizing similar antigens. Analysis of somatic mutations present within the VH genes is also consistent with antigen binding stimulating the growth of these lymphomas.


Proceedings of the National Academy of Sciences of the United States of America | 1992

Clonal evolution of a follicular lymphoma: evidence for antigen selection

David W. Bahler; Ronald Levy


Blood | 1997

Ongoing Ig Gene Hypermutation in Salivary Gland Mucosa-Associated Lymphoid Tissue-Type Lymphomas

David W. Bahler; John A. Miklos; Steven H. Swerdlow


Blood | 1998

Clonal Salivary Gland Infiltrates Associated With Myoepithelial Sialadenitis (Sjögren's Syndrome) Begin as Nonmalignant Antigen-Selected Expansions

David W. Bahler; Steven H. Swerdlow


Blood | 1991

Ig VH gene expression among human follicular lymphomas.

David W. Bahler; Michael J. Campbell; Sarah Hart; Richard A. Miller; Shoshana Levy; Ronald Levy


Journal of Investigative Dermatology | 1993

Transformation of Mycosis Fungoides: T-Cell Receptor β Gene Analysis Demonstrates a Common Clonal Origin for Plaque-Type Mycosis Fungoides and CD30+ Large-Cell Lymphoma

Gary S. Wood; David W. Bahler; Richard T. Hoppe; Roger A. Warnke; Jeffrey Sklar; Ronald Levy


American Journal of Pathology | 1992

Diversity of T-cell antigen receptor variable genes used by mycosis fungoides cells.

David W. Bahler; Gerald J. Berry; Jorge R. Oksenberg; Roger A. Warnke; Ronald Levy


Cancer Research | 1992

Antigen Selection in Human Lymphomagenesis

David W. Bahler; Andrew D. Zelenetz; Thomas T. Chen; Ronald Levy


Annals of Oncology | 1991

Follicular lymphoma: A model of lymphoid tumor progression in man

Andrew D. Zelenetz; Michael J. Campbell; David W. Bahler; S Takahashi; Rachel Oren; Laura Esserman; Dale T. Umetsu; Larry W. Kwak; David G. Maloney; S Brown; Thomas T. Chen; M L Andria; Shoshana Levy; Richard A. Miller; Ronald Levy

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Andrew D. Zelenetz

Memorial Sloan Kettering Cancer Center

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John A. Miklos

University of Pittsburgh

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