Cytosolic low molecular weight acid phosphatase (ACP1) is a high polymorphic phosphotyrosine-protein-phosphatase involved in signal transduction. In NIDDM subjects we have found that ACP1 genotype is a highly significant predictor of retinopathy, suggesting that genetic variability of signal transduction may have an important role in the susceptibility to this complication. Adenosine deaminase, ABO blood groups and several clinical variables have been also considered. The results point out the importance of interactions between genetic systems. Among non-genetic variables dislipidemia and treatment with insulin are significantly associated with retinopathy.

Lucarini, N., Bottini, N., Antonacci, E., Borgiani, P., Faggioni, G., Gloria Bottini, F. (1997). Diabetic complications and the genetics of signal transduction. A study of retinopathy in NIDDM. DISEASE MARKERS, 13(3), 169-176.

Diabetic complications and the genetics of signal transduction. A study of retinopathy in NIDDM

BOTTINI, NUNZIO;BORGIANI, PAOLA;
1997-01-01

Abstract

Cytosolic low molecular weight acid phosphatase (ACP1) is a high polymorphic phosphotyrosine-protein-phosphatase involved in signal transduction. In NIDDM subjects we have found that ACP1 genotype is a highly significant predictor of retinopathy, suggesting that genetic variability of signal transduction may have an important role in the susceptibility to this complication. Adenosine deaminase, ABO blood groups and several clinical variables have been also considered. The results point out the importance of interactions between genetic systems. Among non-genetic variables dislipidemia and treatment with insulin are significantly associated with retinopathy.
1997
Pubblicato
Rilevanza internazionale
Articolo
Sì, ma tipo non specificato
Settore MED/03 - GENETICA MEDICA
English
Lucarini, N., Bottini, N., Antonacci, E., Borgiani, P., Faggioni, G., Gloria Bottini, F. (1997). Diabetic complications and the genetics of signal transduction. A study of retinopathy in NIDDM. DISEASE MARKERS, 13(3), 169-176.
Lucarini, N; Bottini, N; Antonacci, E; Borgiani, P; Faggioni, G; Gloria Bottini, F
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/103588
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