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      Distribución de las frecuencias alélicas y genotípicas del polimorfismo GHRd3 en pacientes venezolanos con talla baja

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          Abstract

          Objetivos. La deleción (GHRd3) o inserción (GHRfl) del exón 3 es un polimorfismo común en el gen del receptor de la hormona de crecimiento (GHR) en los seres humanos. La presencia del alelo GHRd3 se ha asociado con el grado de respuesta de terapia con Hormona de Crecimiento Recombinante Humana (rhGH). El objetivo de este estudio fue determinar las frecuencias alélicas y genotípicas de este polimorfismo en un grupo de 69 niños venezolanos con talla baja que estaban recibiendo rhGH. Métodos. Se extrajo DNA a través de la técnica del método combinado Fenol/Sevag e Inorgánica. Se determinó el genotipo del exón 3 del gen GHR usando tanto PCR- monoplex como PCR-multiplex. Resultados. Entre los pacientes con talla baja la frecuencia genotípica se distribuyó de la siguiente manera: GHRfl/GHRfl (55%) GHRfl/GHRd3 (35%) y GHRd3/GHRd3 (10%) y la frecuencia alélica fue de 0,27 para GHRd3 y 0,73 para GHRfl. Para el grupo testigo la frecuencia genotípica se distribuyo así: GHRfl/GHRfl (56%), GHRfl/ GHRd3 (30%) y GHRd3/GHRd3 (14%) y la frecuencia alélica era de 0,29 para GHRd3 y 0,71 para GHRfl. Las características clínicas basales de los pacientes con talla baja eran similares entre los diferentes genotipos encontrados en el grupo de estudio. Conclusiones. La proporción del genotipo y los alelos del gen GHR fueron similares entre el grupo testigo y los pacientes con talla baja, lo que traduce que la etiología de la talla baja no obedece a este polimorfismo.

          Translated abstract

          Objective. The deletion (GHRd3) or insertion (GHRfl) of exon 3 is a common polymorphism in the receptor growth hormone gene (GHR) in humans. The presence of the allele GHRd3 has been associated with the degree of responsiveness to therapy with recombinant human Growth Hormone (rhGH). The aim of this study was to determine the genotypic and allele frequencies of this polymorphism in a group of 69 Venezuelan children with short stature who were receiving rhGH. Methods. Genomic DNA was extracted from blood lymphocytes using combined method Fenol/SEVAG + Salting out. The GHR-exon 3 was genotyped using both PCR monoplex and multiplex assays. Results. Among patients with short stature, genotype frequency was distributed as follows: GHRfl/GHRfl (55%), GHRfl/GHRd3 (35%) and GHRd3/GHRd3 (10%) and allele frequency for GHRd3 and GHRfl was 0.27 and 0.73, respectively. For the control group, genotype frequency was distributed as follows: GHRfl/GHRfl (56%), GHRfl/GHRd3 (30%) and GHRd3/GHRd3 (14%) and allele frequency for GHRd3 and GHRfl was 0.29 and 0.71, respectively. The baseline clinical features of patients with short stature were similar among different genotypes found in the study group. Conclusions. The proportion of genotype and allele of the GHR gene were similar between the control group and patients with short stature, which translates that the etiology of short stature is not due to this polymorphism.

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          Laron syndrome (primary growth hormone resistance or insensitivity): the personal experience 1958-2003.

          Zvi Laron (2004)
          Clinical and laboratory investigations starting in 1958 of a group of dwarfed children resembling isolated GH deficiency but who had very high serum levels of GH led to the description of the syndrome of primary GH resistance or insensitivity (Laron syndrome) and subsequently to the discovery of its molecular defects residing in the GH receptor and leading to an inability of IGF-I generation. With the biosynthesis of IGF-I in 1986, therapeutic trials started. Continuously more and more patients are being diagnosed in many parts of the world with a variety of molecular defects. This syndrome proved to be a unique model that enables the study of the consequences of GH receptor defects, the physiopathology of GH-IGF-I disruption, and comparison of the GH-independent IGF-I effects. This review presents the personal experience gained from the study follow-up and treatment of the 60 patients followed up for many years in the Israeli cohort.
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            A common polymorphism of the growth hormone receptor is associated with increased responsiveness to growth hormone.

            Christine Dos Santos, Laurent Essioux, Cécile Teinturier (2004)
            Growth hormone is used to increase height in short children who are not deficient in growth hormone, but its efficacy varies largely across individuals. The genetic factors responsible for this variation are entirely unknown. In two cohorts of short children treated with growth hormone, we found that an isoform of the growth hormone receptor gene that lacks exon 3 (d3-GHR) was associated with 1.7 to 2 times more growth acceleration induced by growth hormone than the full-length isoform (P < 0.0001). In transfection experiments, the transduction of growth hormone signaling through d3-GHR homo- or heterodimers was approximately 30% higher than through full-length GHR homodimers (P < 0.0001). One-half of Europeans are hetero- or homozygous with respect to the allele encoding the d3-GHR isoform, which is dominant over the full-length isoform. These observations suggest that the polymorphism in exon 3 of GHR is important in growth hormone pharmacogenetics.
            Article 0 comments Cited 62 times – based on 0 reviews     Review now
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              Height velocity targets from the national cooperative growth study for first-year growth hormone responses in short children.

              Ron Rosenfeld, Bert Bakker, Henry Anhalt (2008)
              Although GH has been used to treat short stature in GH deficiency (GHD) and other conditions for more than 40 yr, criteria for satisfactorily defining targets for GH responsiveness have never been developed. The objective of this study was to present the first-year growth expressed as height velocity (HV) for prepubertal boys and girls with idiopathic GHD, organic GHD, idiopathic short stature, or Turner syndrome from Genentech's National Cooperative Growth Study to derive age-specific targets for GH responsiveness for each etiology and gender. Using data from the National Cooperative Growth Study, we constructed curves of response to GH during the first year of treatment with standard daily doses in naive-to-treatment prepubertal children with idiopathic GHD (2323 males, 842 females), organic GHD (582 males, 387 females), idiopathic short stature (1392 males, 465 females), or Turner syndrome (1367 females). For each category, mean pretreatment and mean +/-1 and +/-2 sd for the first-year HV on GH were assessed. Mean and mean +/- 1 sd for HV were plotted vs. age at baseline (initiation of GH treatment) and compared with mean pretreatment HV. HV plots for each category as a factor of age at baseline are presented. Mean - 2 sd HV plots approximated the pretreatment HV. Using baseline age- and gender-specific targets will assist clinicians in assessing a patient's first-year growth response. We propose that HV below the mean - 1 sd on these plots be considered a "poor" response. These curves may be used to identify patients who may benefit from GH dose adjustment, to assess compliance issues, or to challenge the original diagnosis.
              Article 0 comments Cited 51 times – based on 0 reviews     Review now
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                Author and article information

                Contributors
                Francisco Álvarez-Nava: Role: ND
                Roberto Lanes: Role: ND
                Henry Marcano: Role: ND
                Tatiana Pardo: Role: ND
                William Zabala: Role: ND
                José M Quintero: Role: ND
                Mariela Paoli: Role: ND
                Peter Gunczler: Role: ND
                Nora Maulino: Role: ND
                Marvelys Pérez: Role: ND
                Karilé Méndez: Role: ND
                Marisol Soto: Role: ND
                Ernesto Solís: Role: ND
                Joalice Villalobos: Role: ND
                Journal
                Journal ID (publisher): rvdem
                Title: Revista Venezolana de Endocrinología y Metabolismo
                Abbreviated Title: Rev. Venez. Endocrinol. Metab.
                Publisher: Sociedad Venezolana de Endocrinología y Metabolismo (Mérida )
                ISSN: 1690-3110
                Publication date (Print): February 2009
                Volume: 7
                Issue: 1
                Pages: 26-34
                Affiliations
                [1 ] Universidad del Zulia Venezuela
                [2 ] Hospital de Clínicas Caracas Venezuela
                [3 ] Hospital de Niños J.M. de Los Ríos Venezuela
                [4 ] Universidad de Los Andes Venezuela
                [5 ] Hospital de Especialidades Pediátricas de Maracaibo Venezuela
                Article
                Publisher ID: S1690-31102009000100004
                SO-VID: d31074ec-c837-40c2-a091-8404c0e18937
                License:

                http://creativecommons.org/licenses/by/4.0/

                History
                Product

                SciELO Venezuela

                Self URI (journal page): http://www.scielo.org.ve/scielo.php?script=sci_serial&pid=1690-3110&lng=en
                Categories
                Subject: ENDOCRINOLOGY & METABOLISM

                ScienceOpen disciplines: Endocrinology & Diabetes
                Keywords: Allele and Genotype Frecuencies,GHR gene,Growth Hormone Deficiency,Hardy-Weinberg Equilibrium,Polymorphism,Short Stature,Deficiencia de Hormona de Crecimiento,Equilibrio de Hardy-Weinberg,Frecuencia Alélica y Genotípica,gen GHR,Polimorfismo,Talla Baja
                Data availability:
                ScienceOpen disciplines: Endocrinology & Diabetes
                Keywords: Allele and Genotype Frecuencies, GHR gene, Growth Hormone Deficiency, Hardy-Weinberg Equilibrium, Polymorphism, Short Stature, Deficiencia de Hormona de Crecimiento, Equilibrio de Hardy-Weinberg, Frecuencia Alélica y Genotípica, gen GHR, Polimorfismo, Talla Baja

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