Activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant

Activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant

Changes at the invariable donor splice site +. 1 guanine, relatively frequent in human genetic disease, are predicted to abrogate correct splicing, and thus are classified as null mutations. However, their ability to direct residual expression, which might have pathophysiological implications in sev...

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Main Authors: Nicola Cavallari, Dario Balestra, Alessio Branchini, Iva Maestri, Ampaiwan Chuamsunrit, Werasak Sasanakul, Guglielmo Mariani, Franco Pagani, Francesco Bernardi, Mirko Pinotti
Other Authors: University of Ferrara
Format: Article
Published: 2018
Subjects:
Biochemistry, Genetics and Molecular Biology
Online Access:https://repository.li.mahidol.ac.th/handle/123456789/13677
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spelling th-mahidol.136772018-06-11T11:35:40Z Activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant Nicola Cavallari Dario Balestra Alessio Branchini Iva Maestri Ampaiwan Chuamsunrit Werasak Sasanakul Guglielmo Mariani Franco Pagani Francesco Bernardi Mirko Pinotti University of Ferrara Mahidol University Universita degli Studi dell'Aquila International Centre for Genetic Engineering and Biotechnology Biochemistry, Genetics and Molecular Biology Changes at the invariable donor splice site +. 1 guanine, relatively frequent in human genetic disease, are predicted to abrogate correct splicing, and thus are classified as null mutations. However, their ability to direct residual expression, which might have pathophysiological implications in several diseases, has been poorly investigated. As a model to address this issue, we studied the IVS6. +. 1G. > . T mutation found in patients with severe deficiency of the protease triggering coagulation, factor VII (FVII), whose absence is considered lethal. In expression studies, the IVS6. +. 1G. > . T induced exon 6 skipping and frame-shift, and prevented synthesis of correct FVII transcripts detectable by radioactive/fluorescent labelling or real-time RT-PCR. Intriguingly, the mutation induced the activation of a cryptic donor splice site in exon 6 and production of an in-frame 30. bp deleted transcript (8. ±. 2%). Expression of this cDNA variant, lacking 10 residues in the activation domain, resulted in secretion of trace amounts (0.2. ±. 0.04%) of protein with appreciable specific activity (48. ±. 16% of wt-FVII). Altogether these data indicate that the IVS6. +. 1G. > . T mutation is compatible with the synthesis of functional FVII molecules (~. 0.01% of normal, 1. pM), which could trigger coagulation. The low but detectable thrombin generation (352. ±. 55. nM) measured in plasma from an IVS6. +. 1G. > . T homozygote was consistent with a minimal initiation of the enzymatic cascade. In conclusion, we provide experimental clues for traces of FVII expression, which might have reverted an otherwise perinatally lethal genetic condition. © 2012 Elsevier B.V. 2018-06-11T04:35:40Z 2018-06-11T04:35:40Z 2012-07-01 Article Biochimica et Biophysica Acta - Molecular Basis of Disease. Vol.1822, No.7 (2012), 1109-1113 10.1016/j.bbadis.2012.03.001 1879260X 09254439 2-s2.0-84860335481 https://repository.li.mahidol.ac.th/handle/123456789/13677 Mahidol University SCOPUS https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=84860335481&origin=inward
institution Mahidol University
building Mahidol University Library
continent Asia
country Thailand
Thailand
content_provider Mahidol University Library
collection Mahidol University Institutional Repository
topic Biochemistry, Genetics and Molecular Biology
spellingShingle Biochemistry, Genetics and Molecular Biology
Nicola Cavallari
Dario Balestra
Alessio Branchini
Iva Maestri
Ampaiwan Chuamsunrit
Werasak Sasanakul
Guglielmo Mariani
Franco Pagani
Francesco Bernardi
Mirko Pinotti
Activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant
description Changes at the invariable donor splice site +. 1 guanine, relatively frequent in human genetic disease, are predicted to abrogate correct splicing, and thus are classified as null mutations. However, their ability to direct residual expression, which might have pathophysiological implications in several diseases, has been poorly investigated. As a model to address this issue, we studied the IVS6. +. 1G. > . T mutation found in patients with severe deficiency of the protease triggering coagulation, factor VII (FVII), whose absence is considered lethal. In expression studies, the IVS6. +. 1G. > . T induced exon 6 skipping and frame-shift, and prevented synthesis of correct FVII transcripts detectable by radioactive/fluorescent labelling or real-time RT-PCR. Intriguingly, the mutation induced the activation of a cryptic donor splice site in exon 6 and production of an in-frame 30. bp deleted transcript (8. ±. 2%). Expression of this cDNA variant, lacking 10 residues in the activation domain, resulted in secretion of trace amounts (0.2. ±. 0.04%) of protein with appreciable specific activity (48. ±. 16% of wt-FVII). Altogether these data indicate that the IVS6. +. 1G. > . T mutation is compatible with the synthesis of functional FVII molecules (~. 0.01% of normal, 1. pM), which could trigger coagulation. The low but detectable thrombin generation (352. ±. 55. nM) measured in plasma from an IVS6. +. 1G. > . T homozygote was consistent with a minimal initiation of the enzymatic cascade. In conclusion, we provide experimental clues for traces of FVII expression, which might have reverted an otherwise perinatally lethal genetic condition. © 2012 Elsevier B.V.
author2 University of Ferrara
author_facet University of Ferrara
Nicola Cavallari
Dario Balestra
Alessio Branchini
Iva Maestri
Ampaiwan Chuamsunrit
Werasak Sasanakul
Guglielmo Mariani
Franco Pagani
Francesco Bernardi
Mirko Pinotti
format Article
author Nicola Cavallari
Dario Balestra
Alessio Branchini
Iva Maestri
Ampaiwan Chuamsunrit
Werasak Sasanakul
Guglielmo Mariani
Franco Pagani
Francesco Bernardi
Mirko Pinotti
author_sort Nicola Cavallari
title Activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant
title_short Activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant
title_full Activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant
title_fullStr Activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant
title_full_unstemmed Activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant
title_sort activation of a cryptic splice site in a potentially lethal coagulation defect accounts for a functional protein variant
publishDate 2018
url https://repository.li.mahidol.ac.th/handle/123456789/13677
_version_ 1763495833553076224

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