The insulin receptor () gene was analyzed in four patients with severe insulin resistance, revealing five novel mutations and a deletion that removed exon 2. A patient with Donohue syndrome (DS) had a novel p.V657F mutation in the second fibronectin type III domain (FnIII-2), which contains the α-β cleavage site and part of the insulin-binding site. The mutant INSR was expressed in Chinese hamster ovary cells, revealing that it reduced insulin proreceptor processing and impaired activation of downstream signaling cascades. Using online databases, we analyzed 82 missense mutations and demonstrated that mutations causing DS were more frequently located in the FnIII domains than those causing the milder type A insulin resistance ( = 0.016). In silico structural analysis revealed that missense mutations predicted to severely impair hydrophobic core formation and stability of the FnIII domains all caused DS, whereas those predicted to produce localized destabilization and to not affect folding of the FnIII domains all caused the less severe Rabson-Mendenhall syndrome. These results suggest the importance of the FnIII domains, provide insight into the molecular mechanism of severe insulin resistance, will aid early diagnosis, and will provide potential novel targets for treating extreme insulin resistance.
Abstract.We performed genetic analysis and clinical investigations for three patients with
suspected monocarboxylate transporter 8 (MCT8) deficiency. On genetic analysis of the
MCT8(SLC16A2) gene, novel mutations (c.1333C>A;
p.R445S, c.587G>A; p.G196E and c.1063_1064insCTACC; p.R355PfsX64) were identified in
each of three patients. Although thyroid function tests (TFTs) showed the typical pattern
of MCT8 deficiency at the time of genetic diagnosis in all patients, two patients
occasionally were euthyroid. A TRH test revealed low response, exaggerated response and
normal response of TSH, respectively. Endocrinological studies showed gonadotropin (Gn)
deficiency in two adult patients. On ultrasonography, goiter was detected in one patient.
Interestingly, pituitary magnetic resonance imaging (MRI) demonstrated atrophy and
thinness of the pituitary gland in two patients. Our findings suggest that thyroid status
in patients with MCT8 deficiency varies with time of examination, and repeated TFTs are
necessary for patients suspected of MCT8 deficiency before genetic analysis. In addition,
it is noteworthy that some variations were observed on the TRH test and ultrasonography of
the thyroid gland in the present study. Morphological abnormality of the pituitary gland
may be found in some patients, while Gn deficiency should be considered as one of the
complications.
A nine-month-old boy, with functional disomy for Xq26-qter and multiple congenital abnormalities, is reported. The boy had severe pre- and postnatal growth retardation, profound developmental delay, hypotonia, microcephaly, agenesis of the corpus callosum, dysmorphic facial features, cryptorchidism, and left multidysplastic kidney. He developed feeding difficulties and infantile spasms. G-banding analysis of his chromosomes showed additional material on the short arm of chromosome 21. His parents refused to submit to chromosome analysis. Analysis with chromosome microdissection followed by reverse and forward chromosome painting indicated his karyotype as 46,XY,der(21)t(X;21)(q26;p11.2). This is the first description of pure functional disomy for Xq26-qter due to an unbalanced X-autosome translocation.
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