The identification of a Btk mutation in a male patient with < 2% CD19+ B cells warrants making the diagnosis of X-linked Agammaglobulinemia (XLA). Herein we report the case of a 31 year-old male with a gradual decline of peripheral B lymphocytes and low IgA and IgM but normal IgG levels. His clinical history revealed recurrent respiratory and skin infections, sclerosing cholangitis and chronic obstructive pancreatitis. Molecular studies revealed a novel aminoacidic substitution in Btk protein (T316A). His mother, maternal aunts and a maternal female cousin were heterozygotes for the same Btk mutation and were variably affected with pulmonary emphysema. This is a puzzling case where the patient's clinical history and laboratory findings divorce molecular genetics. Either this case confirms the variable expressivity of XLA disease or the T316A change in Btk SH2 domain is a novel non-pathogenic mutation and another unknown gene alteration is responsible for the disease.

Graziani, S., DI MATTEO, G., Benini, L., Di Cesare, S., Chiriaco, M., Chini, L., et al. (2008). Identification of a Btk mutation in a dysgammaglobulinemic patient with reduced B cells: XLA diagnosis or not?. CLINICAL IMMUNOLOGY, 128, 322-328 [10.1016/j.clim.2008.05.012].

Identification of a Btk mutation in a dysgammaglobulinemic patient with reduced B cells: XLA diagnosis or not?

DI MATTEO, GIGLIOLA;CHINI, LOREDANA;ROSSI, PAOLO;MOSCHESE, VIVIANA
2008-09-01

Abstract

The identification of a Btk mutation in a male patient with < 2% CD19+ B cells warrants making the diagnosis of X-linked Agammaglobulinemia (XLA). Herein we report the case of a 31 year-old male with a gradual decline of peripheral B lymphocytes and low IgA and IgM but normal IgG levels. His clinical history revealed recurrent respiratory and skin infections, sclerosing cholangitis and chronic obstructive pancreatitis. Molecular studies revealed a novel aminoacidic substitution in Btk protein (T316A). His mother, maternal aunts and a maternal female cousin were heterozygotes for the same Btk mutation and were variably affected with pulmonary emphysema. This is a puzzling case where the patient's clinical history and laboratory findings divorce molecular genetics. Either this case confirms the variable expressivity of XLA disease or the T316A change in Btk SH2 domain is a novel non-pathogenic mutation and another unknown gene alteration is responsible for the disease.
1-set-2008
Pubblicato
Rilevanza internazionale
Articolo
Esperti anonimi
Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA
English
Con Impact Factor ISI
XLA; Btk; Sclerosing cholangitis; Chronic obstructive pancreatitis
Graziani, S., DI MATTEO, G., Benini, L., Di Cesare, S., Chiriaco, M., Chini, L., et al. (2008). Identification of a Btk mutation in a dysgammaglobulinemic patient with reduced B cells: XLA diagnosis or not?. CLINICAL IMMUNOLOGY, 128, 322-328 [10.1016/j.clim.2008.05.012].
Graziani, S; DI MATTEO, G; Benini, L; Di Cesare, S; Chiriaco, M; Chini, L; Chianca, M; De Iorio, F; La Rocca, M; Iannini, R; Corrente, S; Rossi, P; Mo...espandi
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/48088
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