CEDIE   05498
CENTRO DE INVESTIGACIONES ENDOCRINOLOGICAS "DR. CESAR BERGADA"
Unidad Ejecutora - UE
congresos y reuniones científicas
Título:
Pediatric Non Autoimmune Hyperthyrotropinemia and TSH Receptor Gene (TSHR) Variants
Autor/es:
SCAGLIA, P.A; KESELMAN, ANA; GRUÑEIRO PAPENDIECK, L; PAPENDIECK P; BERGADÁ, I; DOMENÉ, HORACIO; CHIESA, A.
Lugar:
Playa del Carmen
Reunión:
Congreso; XXIV Reuniòn de la Sociedad Latinoamericana de Endocrinología Pediátrica; 2014
Institución organizadora:
Sociedad Latinoamericana de Endocrinoologia Pediatrica
Resumen:
Introduction: Mild TSH resistance characterized by non auto- immune hyperthyrotropinemia (NAH) has been described associ- ated with heterozygous variants in TSHR gene. The prevalence of this condition varies in different reports and its occurrence is con- sidered when subclinical hypothyroidism is assessed. Objective: To study the prevalence of TSHR gene variants in a pediatric population with NAH. Subjects and Methods: Thirty five non obese unrelated chil- dren with NAH (18 girls), aged 1 to 19 years, were enrolled. Eigh- teen patients were born small for gestational age (SGA). All pre- sented at least two TSH measurements >5 mIU/L (median 8.8, range 5.7?14.0 mIU/L), with normal total (T4) and free thyroxine (FT4) and negative ATPO and ATG anti-thyroid antibodies. Se- rum levels of TSH, T4 and FT4 were measured by ECLIA method and ATPO and ATG antibodies by ICMA (Immulite). The whole coding sequence of TSHR gene (exons 1 to 10 and intronic flank- ing regions) was PCR amplified from genomic DNA and auto- matically sequenced. Polyphen 2, SIFT and Mutation Taster soft- wares were used for in silico prediction of gene variants effects. Results: Several known polymorphic variants were found (al- lelic frequency): p.Pro52Thr (4.3%), p.Asn187Asn (14.3%), p. Ala459Ala (1.4%), p.Asp727Glu (15.7%) and p.Asn744Lys (1.4%). In two patients, both non SGA, two uncommon heterozygous vari- ants were found in exon 10. Both variants were predicted as patho- genic by three different prediction softwares. Patient 1 and his fa- ther carried the novel p.Pro407Leu (c.1220C>T) missense variant, present with very low allelic frequency (1/13005) only in Exome variant server database [1]. Patient 2, his father and brother carried the p.Ile583Thr (c.1748T>C) variant, absent in available popula- tion databases but already reported in one NAH patient and de- scribed as less responsive to TSH stimulation in vitro than the wild type receptor. In vitro expression of the novel p.Pro407Leu variant is required to establish its role in thyroid pathogenesis. Conclusions: In a relatively small cohort of pediatric patients with NAH we were able to find ~6% of potential pathogenic TSHR gene variants. Nevertheless, further investigation is needed to as- sess their deleterious effect on thyroid function and to apply this knowledge to the clinical management of pediatric subclinical hy- pothyroidism. References 1 Exome Variant Server, NHLBI GO Exome Sequencing Project (ESP), Seattle, WA (URL: http://evs.gs.washington.edu/EVS/) [june, 2014]. 2 Calebiro D, et al: JCEM. 2012;97:E156?E160.