CAIO ROBLEDO D'ANGIOLI COSTA QUAIO
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- Tegumentary manifestations of Noonan and Noonan-related syndromes(2013) QUAIO, Caio Robledo D'Angioli Costa; ALMEIDA, Tatiana Ferreira de; BRASIL, Amanda Salem; PEREIRA, Alexandre C.; JORGE, Alexander A. L.; MALAQUIAS, Alexsandra C.; KIM, Chong Ae; BERTOLA, Debora RomeoOBJECTIVES: Noonan and Noonan-related syndromes are common autosomal dominant disorders with neuro-cardio-facial-cutaneous and developmental involvement. The objective of this article is to describe the most relevant tegumentary findings in a cohort of 41 patients with Noonan or Noonan-related syndromes and to detail certain aspects of the molecular mechanisms underlying ectodermal involvement. METHODS: A standard questionnaire was administered. A focused physical examination and a systematic review of clinical records was performed on all patients to verify the presence of tegumentary alterations. The molecular analysis of this cohort included sequencing of the following genes in all patients: PTPN1, SOS1, RAF1, KRAS, SHOC2 and BRAF. RESULTS: The most frequent tegumentary alterations were xeroderma (46%), photosensitivity (29%), excessive hair loss (24%), recurrent oral ulcers (22%), curly hair (20%), nevi (17%), markedly increased palmar and plantar creases (12%), follicular hyperkeratosis (12%), palmoplantar hyperkeratosis (10%), cafe-au-lait spots (10%) and sparse eyebrows (7%). Patients with mutations in PTPN11 had lower frequencies of palmar and plantar creases and palmar/plantar hyperkeratosis compared with the other patients. CONCLUSIONS: We observed that patients with mutations in genes directly involved in cell proliferation kinase cascades (SOS1, BRAF, KRAS and RAF1) had a higher frequency of hyperkeratotic lesions compared with patients with mutations in genes that have a more complex interaction with and modulation of cell proliferation kinase cascades (PTPN11).
bookPart Abordagem genético-clínica na síndrome de Down(2013) QUAIO, Caio Robledo D'Angioli Costa; KIM, Chong Ae- A Dominant ABCC8-Related Hyperinsulinism: Familial Case Report Moreira et al. ABCC8-Related Hyperinsulinism(2013) MOREIRA, M. C.; PIAZZON, F. B.; CARVALHO, M. D. F.; QUAIO, C. R. D. C.; DUTRA, A. B.; CECCON, M. E.; DELLA-MANNA, T.; TANNURI, U.; LEE, J. H.; ZERBINI, M. C. N.; BELLANNE-CHANTELOT, C.; LONLAY, P.; BERTOLA, D. R.; KIM, C. A.
- Vertical transmission of a frontonasal phenotype caused by a novel ALX4 mutation(2013) BERTOLA, Debora R.; RODRIGUES, Melina G.; QUAIO, Caio R. D. C.; KIM, Chong A.; PASSOS-BUENO, Maria RitaFrontonasal dysplasias (FND) comprise a spectrum of disorders caused by abnormal median facial development. Its etiology is still poorly understood but recently frontonasal dysplasia phenotypes were linked to loss-of-function mutations in the ALX homeobox gene family, which comprises the ALX1, ALX3, and ALX4 genes. All ALX-related frontonasal phenotypes till date had been compatible with an autosomal recessive mode of inheritance. In contrast, heterozygous loss-of-function mutations in ALX4 had been only associated with isolated symmetrical parietal ossification defects at the intersection of the sagittal and lambdoid sutures, known as enlarged parietal foramina. We report a family with vertical transmission from mother to son of mild frontonasal dysplasia phenotype caused by a novel ALX4 gene mutation (c.1080-1089_delGACCCGGTGCinsCTAAGATCTCAACAGAGATGGCAACT, p.Asp326fsX21).This is the first report of a frontonasal phenotype related to a heterozygous mutation in ALX4. This mutation is predicted to cause the loss of the aristaless domain in the C-terminal region of the protein and preserves the homeodomain. We speculate that a different mechanism, a dominant-negative effect, is responsible for the distinct phenotype in this family. (c) 2013 Wiley Periodicals, Inc.