Your search keyword '"Loss of function mutation"' showing total 3 results

1. Molecular and cellular basis of hypophosphatasia.

Author

Komaru, Keiichi, Ishida-Okumura, Yoko, Numa-Kinjoh, Natsuko, Hasegawa, Tomoka, and Oda, Kimimitsu

Abstract

Hypophosphatasia (HPP) is an inherited disorder characterized by defective mineralization of the bone and teeth that is also associated with a deficiency of serum alkaline phosphatase (ALP). Patients with HPP exhibit a broad range of symptoms including stillbirth with an unmineralized skeleton, premature exfoliation and dental caries in childhood, and pseudo-fractures in adulthood. The broad clinical spectrum of HPP is attributed to various mutations in the ALPL gene, which encodes tissue-nonspecific alkaline phosphatase (TNSALP). Nevertheless, the molecular mechanisms underlying the genotypic and phenotypic relationship of HPP remain unclear. The expression of HPP-related TNSALP mutants in mammalian cells allows us to determine for the effects of mutations on the properties of TNSALP, which could contribute to a better understanding of the relationship between structure and function of TNSALP. Molecular characterization of TNSALP mutants helps establish the etiology and onset of HPP. [ABSTRACT FROM AUTHOR]

Published

2019

2. TP53 mutations in high grade serous ovarian cancer and impact on clinical outcomes: a comparison of next generation sequencing and bioinformatics analyses.

Author

Mandilaras, Victoria, Garg, Swati, Cabanero, Michael, Tan, Qian, Pastrello, Chiara, Burnier, Julia, Karakasis, Katherine, Wang, Lisa, Neesha, C Dhani, Marcus, O Butler, Philippe, L Bedard, Lillian, L Siu, Clarke, Blaise, Patricia, Ann Shaw, Stockley, Tracy, Jurisica, Igor, Amit, M Oza, and Lheureux, Stephanie

Subjects

GENETIC mutation, OVARIAN cancer, CLINICAL trials, NUCLEOTIDE sequencing, BIOINFORMATICS

Abstract

Objective: Mutations in TP53 are found in the majority of high grade serous ovarian cancers, leading to gain of function or loss of function of its protein product, p53, involved in oncogenesis. There have been conflicting reports as to the impact of the type of these on prognosis. We aim to further elucidate this relationship in our cohort of patients. Methods: 229 patients with high grade serous ovarian cancer underwent tumor profiling through an institutional molecular screening program with targeted next generation sequencing. TP53 mutations were classified using methods previously described in the literature. Immunohistochemistry on formalin-fixed paraffin embedded tissue was used to assess for TP53 mutation. Using divisive hierarchal clustering, we generated patient clusters with similar clinicopathologic characteristics to investigate differences in outcomes. Results: Six different classification schemes of TP53 mutations were studied. These did not show an association with first platinum-free interval or overall survival. Next generation sequencing reliably predicted mutation in 80% of cases, similar to the proportion detected by immunohistochemistry. Divisive hierarchical clustering generated four main clusters, with cluster 3 having a significantly worse prognosis (p<0.0001; log-rank test). This cluster had a higher concentration of gain of function mutations and these patients were less likely to have undergone optimal debulking surgery. Conclusions: Different classifications of TP53 mutations did not show an impact on outcomes in this study. Immunohistochemistry was a good predictor for TP53 mutation. Cluster analysis showed that a subgroup of patients with gain of function mutations (cluster 3) had a worse prognosis. [ABSTRACT FROM AUTHOR]

Published

2019

3. Marie Unna hereditary hypotrichosis: Identification of a U2HR mutation in the family from the original 1925 report.

Author

Redler, Silke, Kruse, Roland, Eigelshoven, Sibylle, Hanneken, Sandra, Refke, Melanie, Wen, Yaran, Zhang, Xue, Cichon, Sven, Betz, Regina C., and Nöthen, Markus M.

Abstract

Background: In 1925, Dr Marie Unna described a rare form of hereditary hypotrichosis in a German multigenerational family. This was later termed “Marie Unna hereditary hypotrichosis” (MUHH). MUHH is an autosomal dominant disorder that is characterized by the absence or scarcity of scalp hair, eyebrows, and eyelashes at birth; coarse and wiry hair during childhood; and progressive hair loss beginning around puberty. Causal mutations in U2HR, an inhibitory upstream open reading frame in the 5''-untranslated region of the human hairless (HR) gene, were recently identified in several unrelated MUHH families from various ethnic backgrounds. Objective: Although there have been several clinical reports of descendants of the originally described family, the molecular cause of disease in this particular family has not been established. The aim of this study was to investigate descendants of this family and to analyze their DNA for the presence of U2HR mutations. Methods: Descendants of the family (including one affected individual) were examined clinically. Direct sequencing of U2HR was performed. Enzymatic digestion using the restriction enzyme NcoI was performed to confirm the sequencing results. Results: The index patient displayed the typical MUHH pattern of hair loss and was found to carry the disease-causing c.3G>A (p.M1I) U2HR mutation. This mutation was not detected in unaffected family members. Limitations: Only one affected family member was investigated. Conclusions: Eighty-five years after the first description of this rare form of alopecia, the disease-causing mutation in the originally reported family has been identified. [Copyright &y& Elsevier]

Published

2011