Alpha-1 antitrypsin and liver disease: mechanisms of injury and novel interventions

Teckman, Jeffrey; Mangalat, Nisha

doi:10.1586/17474124.2014.943187

Cited by 47 publications

(40 citation statements)

References 54 publications

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“…Here, we chose to target Exon V of the human SERPINA1 gene encoding for α1-antitrypsin (AAT). A well described G > A point mutation on base number 31 of this Exon leads to a missense amino acid replacement (E342K) resulting in expression of Z-AAT, which is the underlying cause for clinical severe AAT deficiency18. In order to test whether it was possible to use the G > A point mutation for allele-specific targeting of the Z-AAT allele, we cloned either the 59 bp target sequence of Z-AAT or the target sequence of the normal SERPINA1 allele (M-AAT) into the reporter vector.…”

Section: Resultsmentioning

confidence: 99%

“…Several mutations at the SERPINA1 locus have been described to be the causative for AAT deficiency and particularly the E342K point mutation at the beginning of Exon V is related with a severe clinical course. Patients often present a progressive lung disease, such as chronic obstructive pulmonary disease (COPD) and a fraction of them present variable degrees of chronic liver damage, ranging from mild fibrosis to cirrhosis or even hepatocellular carcinoma18. E342K-AAT is prone to self-agglutination and cannot be properly secreted from hepatocytes in the liver, where accumulation inside the endoplasmic reticulum can cause liver disease, whereas lung disease is a consequence of severely reduced AAT serum-concentration.…”

Section: Discussionmentioning

confidence: 99%

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Improved bi-allelic modification of a transcriptionally silent locus in patient-derived iPSC by Cas9 nickase

Eggenschwiler

Moslem

Fráguas

et al. 2016

Sci Rep

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Homology directed repair (HDR)-based genome editing via selectable long flanking arm donors can be hampered by local transgene silencing at transcriptionally silent loci. Here, we report efficient bi-allelic modification of a silent locus in patient-derived hiPSC by using Cas9 nickase and a silencing-resistant donor construct that contains an excisable selection/counter-selection cassette. To identify the most active single guide RNA (sgRNA)/nickase combinations, we employed a lentiviral vector-based reporter assay to determine the HDR efficiencies in cella. Next, we used the most efficient pair of sgRNAs for targeted integration of an improved, silencing-resistant plasmid donor harboring a piggyBac-flanked puroΔtk cassette. Moreover, we took advantage of a dual-fluorescence selection strategy for bi-allelic targeting and achieved 100% counter-selection efficiency after bi-allelic excision of the selection/counter-selection cassette. Together, we present an improved system for efficient bi-allelic modification of transcriptionally silent loci in human pluripotent stem cells.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Improved bi-allelic modification of a transcriptionally silent locus in patient-derived iPSC by Cas9 nickase

Eggenschwiler

Moslem

Fráguas

et al. 2016

Sci Rep

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“…Результаты недавних исследований показывают, что каскад повреждения клеток запускается в небольшой популяции гепатоцитов, имеющих наибольшее накопление мутантного полимеризованного альфа-1-антитрипсина. Указанные гепатоциты, а их только несколько процентов от общего числа клеток, возможно, имеют повышенную активацию каспазы и повышенную восприимчивость к апоптозу [29,41].…”

Section: обзоры литературыunclassified

Pathophysiological aspects of liver damage in children with alpha-1-antitrypsin deficiency

Волынец

Никитин

2020

Ross. vestn. perinatol. pediatr.

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Alpha-1-antitrypsin deficiency is an autosomal recessive disease characterized by both liver damage and lung disease in children and adults because of a decrease in the serum protein content due to the mutations in the PI (proteinase inhibitor) gene. The majority of liver diseases are associated with a homozygous mutation of the Z allele. There are many variations of clinical manifestations of the liver disease in children with the PI*ZZ genotype. In the neonatal period, liver disease is usually cholestatic; and it is accompanied by a prolonged cholestatic jaundice, skin itching, which can be determined only later (after 6 months), decreased appetite and bad weight gain, hepato- and splenomegaly. The article describes the pathophysiology of liver damage in children with alpha-1-antitrypsin deficiency. The authors provide their recommendations for the management of children with suspected and confirmed alpha-1-antitrypsin deficiency.

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“…4,36 Given the high degree of variability among patients with this same ZZ genotype, it is thought that there is likely to be a large influence of genetic and environmental modifiers on the final development of end-organ injury. 1,25 The recognition of these key steps in the pathophysiology, especially the identification of autophagy as a key pathway, and the first publication of an overall, unified scheme of the injury cascade has driven a new era in therapeutic development aimed at AAT liver disease. 23,25 Studies in the mouse model of AAT deficiency have identified more than 10 compounds that effectively block liver injury, although none are yet approved for human use (►Fig.…”

Section: Pathophysiology Of Aat Disease New Insights and Human Trialsmentioning

confidence: 99%

“…The risk of life-threatening liver disease in children is 3 to 5%, although many children may have self-limited neonatal cholestasis or mild serum aminotransferase elevations. 1,7 In the neonatal period, 20% of ZZ patients present with the "neonatal hepatitis syndrome," which includes cholestatic jaundice, pruritus, poor feeding, poor weight gain, hepatomegaly, and splenomegaly. 7,8 Liver biopsy findings may be highly variable in infants including giant cell transformation, lobular hepatitis, significant steatosis, fibrosis, hepatocellular necrosis, bile duct paucity, or bile duct proliferation.…”

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confidence: 99%

Emerging Concepts and Human Trials in Alpha-1-Antitrypsin Deficiency Liver Disease

Teckman

2017

Semin Liver Dis

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In α-1-antitrypsin (AAT) deficiency, individuals homozygous for the AAT mutant Z gene synthesize large quantities of mutant Z protein in the liver, which folds improperly during biogenesis and is retained within the hepatocytes rather than appropriated secreted. This accumulation of mutant Z protein triggers an intracellular injury cascade causing cell death in the population of hepatocytes with the largest accumulations of Z protein. Hepatocellular proliferation, hepatic fibrosis, and hepatocellular cancer in some individuals can be the result. New insights from basic science studies have now allowed the application of new biotechnologies to this previously untreatable disease. Specifically, drugs designed to accelerate the intracellular removal of the mutant Z protein (autophagy enhancers) and siRNA strategies designed to shut down synthesis of the toxic, mutant Z protein, are now in human trials. Other approaches, such as gene correction, cell therapy, and antifibrotic drugs are in preclinical development.

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Alpha-1 antitrypsin and liver disease: mechanisms of injury and novel interventions

Cited by 47 publications

References 54 publications

Improved bi-allelic modification of a transcriptionally silent locus in patient-derived iPSC by Cas9 nickase

Improved bi-allelic modification of a transcriptionally silent locus in patient-derived iPSC by Cas9 nickase

Pathophysiological aspects of liver damage in children with alpha-1-antitrypsin deficiency

Emerging Concepts and Human Trials in Alpha-1-Antitrypsin Deficiency Liver Disease

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