Juan Ramón González-García scite author profile

Juan Ramón González-García

5Publications

32Citation Statements Received

52Citation Statements Given

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Affiliations

Mexican Social Security Institute, University of Guadalajara, Secretaría de Salud de Jalisco

Publications

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Increased expression of AML1‐a and acquired chromosomal abnormalities in childhood acute lymphoblastic leukemia

Gutiérrez-Angulo

González-García

Meza-Espinoza

et al. 2004

Hematological Oncology

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A semi-quantitative expression analysis of both AML1-a and AML1-total was performed by RT-PCR in 19 children with acute lymphoblastic leukemia (ALL) at diagnosis. AML1-a expression was assessed in 16 bone marrow (BM) and 13 peripheral blood (PB) samples whereas AML1-total was assessed in 17 BM and 16 PB samples. These analyses were also carried out in 15 PB samples of healthy controls. In addition, 18/19 patients were karyotyped: 11 had an unmodified constitutional karyotype (CK) and seven exhibited acquired chromosomal abnormalities (ACA). The expression of AML1-a was significantly increased in BM and PB when compared with the controls (p < 0.013 and p < 0.035, respectively). A significant increase was found in the expression of AML1-a in BM of the ACA group compared with the CK group (p < 0.0009). The expression of AML1-a in BM and PB showed a significant increase in the ACA group compared with controls (p < 0.00001 and p < 0.012, respectively); in contrast, the CK group did not differ from the controls. These observations may mean that the increase of AML1-a favours the progression of leukemia.

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Polymorphisms of seven genes involved in lipid metabolism in an unselected Mexican population

Ríos-González

Luévano-Ortega

Saldaña-Cruz

et al. 2011

J Genet

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Distribution of CYP1A1⁎2A polymorphism in adult patients with acute lymphoblastic leukemia in a Mexican population

Gallegos‐Arreola

González-García

Figuera

et al. 2008

Blood Cells, Molecules, and Diseases

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Chromosome 9qh inversions may not be true inversions

1999

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Genomic instability in a chronic lymphocytic leukemia patient with mono-allelic deletion of the DLEU and RB1 genes

Nava-Rodríguez

Domínguez-Cruz²,

Aguilar-López

et al. 2019

Mol Cytogenet

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BackgroundThe most frequent cytogenetic abnormality detected in chronic lymphocytic leukemia (CLL) patients is the presence of a deletion within the chromosome band 13q14. Deletions can be heterogeneous in size, generally encompassing the DLEU1 and DLEU2 genes (minimal deleted region), but at times also including the RB1 gene. The latter, larger type of deletions are associated with worse prognosis.Genomic instability is a characteristic of most cancers and it has been observed in CLL patients mainly associated with telomere shortening.Case presentationCytogenetic and fluorescence in situ hybridization studies of a CLL patient showed a chromosomal translocation t(12;13)(q15;q14), a mono-allelic 13q14 deletion encompassing both the DLEU and RB1 genes, and genomic instability manifested as chromosomal breaks, telomeric associations, binucleated cells, nucleoplasmic bridges, and micronucleated cells.In conclusion, our CLL patient showed genomic instability in conjunction with a 13q14 deletion of approximately 2.6 megabase pair involving the DLEU and RB1 genes, as well as other genes with potential for producing genomic instability due to haploinsufficiency.

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