Acquired potential N-glycosylation sites within the tumor-specific immunoglobulin heavy chains of B-cell malignancies

01-may-2004 | Revista: Haematologica

Zabalegui N, de Cerio AL, Inogés S, Rodríguez-Calvillo M, Pérez-Calvo J, Hernández M, García-Foncillas J, Martín-Algarra S, Rocha E, Bendandi M.

BACKGROUND AND OBJECTIVES
Among B-cell malignancies, follicular lymphomas (FL) more frequently show acquired, potential N-glycosylation sites (AGS) within tumor-specific immunoglobulin.

The aim of this study was to extend this observation and to evaluate the pattern of presentation of AGS within five different forms of B-cell lymphoma.

DESIGN AND METHODS
We sequenced the tumor-specific immunoglobulin heavy chain variable region fragment, including complementarity-determining regions 2 and 3, of forty-seven consecutive patients with a B-cell malignancy enrolled in idiotype vaccine clinical trials. This sequencing approach is known to allow the identification of most AGS. We then statistically analyzed differences in presentation pattern, in terms of tumor histology, immunoglobulin isotype, AGS location and amino acid composition.

RESULTS
All twenty-four FL cases presented with at least one AGS, whereas the vast majority of four B-cell lymphoma types other than FL did not. The non- FL group of tumors included four cases of Burkitt's lymphoma, six of diffuse large cell lymphoma, seven mantle cell lymphomas and six small lymphocytic lymphomas. Most IgM-bearing follicular lymphoma cases featured their AGS within complementarity-determining region 2, as opposed to those bearing an IgG, which mostly displayed the AGS within complementarity-determining region 3. The vast majority of AGS located within either complementarity-determining region ended with a serine residue, whereas those located within framework regions mostly featured threonine as the last amino acid residue.

INTERPRETATION AND CONCLUSIONS
In our series, all cases of FL had AGS within their tumor-specific immunoglobulin heavy chain variable regions. In contrast, most B-cell malignancies other than FL did not. Further studies are warranted in order to establish the possible meaning of these findings in terms of disease pathogenesis, their diagnostic value in doubtful cases and their potential implications for immunotherapy.

CITA DEL ARTICULO Haematologica. 2004 May;89(5):541-6.

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Nuestros autores

La imagen muestra a la Dra. Susana Inogés Sancho, especialista en terapia celular de la Clínica Universidad de Navarra, con amplia experiencia en el campo.La Dra. Inogés es una de las expertas del área de terapia celular en esta institución, reconocida por su trayectoria en investigación y aplicación de terapias innovadoras.Con una formación sólida en medicina regenerativa, la Dra. Inogés ha liderado investigaciones y aplicaciones clínicas de terapia celular para tratar diversas afecciones, especialmente en el campo de la inmunoterapia celular. Su experiencia ha sido reconocida a nivel internacional.Si busca una especialista de confianza en terapia celular, la Dra. Susana Inogés Sancho es la elección ideal.

Dra. Susana Inogés Sancho Ver Curriculum

Especialista Servicio de Inmunología e Inmunoterapia

Sede Pamplona

Imagen Dr. Salvador Martín Algarra, Departamento de Oncología Médica

Dr. Salvador Martín Algarra Ver Curriculum

Especialista Departamento de Oncología Médica

Sede Pamplona