Survival and FEV<sub>1</sub>Decline in Individuals with Severe Deficiency of α<sub>1</sub>-Antitrypsin

Vreim, Carol E.; Wu, Margaret; Crystal, Ronald G.; Buist, A. Sonia; Burrows, Benjamin; Cohen, Allen B.; Fallat, Robert J.; Gadek, James E.; Rousell, R. H.; Rs, Schwartz; Turino, Gerard M.; Schluchter, Mark D.; Stoller, James K.; Wiedemann, Herbert; Williams, Gary W.; Barrett, David M.; Beck, Gerald J.; Midcalf, V.; Moore, Brian; Sartori, Patricia C. E.; Sherer, Susan; Zhang, R.; Petty, Thomas L.; Tomashefski, Joseph F.; Brantly, Mark; Hildesheim, Jeffrey; Rundquist, Bengt; Sandhaus, Robert A.; Bell, C. William; Berend, J. E.; Begle, B.; Erb, David; Seidman, Jessica C.; Sherman, Stanley W; Cameron, Barbara; Weinberger, Steven E.; Rosenberg, Mireille; Johnston, Ric; Arroliga, Alejandro C.; Meeker, David P.; Mehta, Amit; Laskowski, Daniel; Ryan, Judy; Loftin, J. P.; Johnson, Kristen N.; Kotch, Arthur; Clark, Tannia S.; Epstein, Paul E.; Buono, Pietro; Sandblom, Robert E.; Hert, Richard; DeMaine, J. B.; Colar, L.; Eichenhorn, Michael S.; McMahan, Jonathan; Breite, W. M.; Webb-Johnson, David C.; Corbett, Jonathan; McManus, D. P.; Krowka, Michael J.; Zeiger, Tonya; Prakash, Udaya B. S.; Staats, T.; Strange, Charlie; Baumann, Marc; Judson, Marc A.; Oser, Rachel; Soskel, Norman T.; Smith, Vernon L.; Killian, D. N.; Demicco, William A.; Golden, Lewis A.; Hitchcock, Robyn; Moss, Joel; Chu, S.-C. Q.; McElvaney, Noel G.; Barnes, Peter J.; O’Neil, Kevin M.; Holden, David; Meth, B. M.; Ashburn, Richard W.; Forrester, J. V.; Sarlin, Robert F.; Sen, Rouhin; Walsh, Theodore E.; Jones, Spencer S.; Drake, Janice

doi:10.1164/ajrccm.158.1.9712017

Cited by 385 publications

(80 citation statements)

References 35 publications

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“…Although this study was small, it was enough for the product to gain a license for treatment of patients with the PiZ or null phenotypes [75] in the USA, Canada and parts of Europe. Observational work in the USA has since supported the use of AAT replacement, showing a slower decline in lung function in those with an FEV 1 of 35–49% predicted when receiving AAT augmentation [76]. Similar work in Europe has concurred [77, 78], whilst a Canadian study reported a beneficial effect but failed to show the association with baseline FEV 1 [79].…”

Section: Approaches To Treatmentmentioning

confidence: 99%

Alpha One Antitrypsin Deficiency: From Gene to Treatment

Wood

Stockley

2007

Respiration

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α1-antitrypsin deficiency is a genetic disorder which contributes to the development of chronic obstructive pulmonary disease, bronchiectasis, liver cirrhosis and panniculitis. The discovery of α1-antitrypsin and its function as an antiprotease led to the protease-antiprotease hypothesis, which goes some way to explaining the pathogenesis of emphysema. This article will review the clinical features of α1-antitrypsin deficiency, the genetic mutations known to cause it, and how they do so at a molecular level. Specific treatments for the disorder based on this knowledge will be reviewed, including α1-antitrypsin replacement, gene therapy and possible future therapies, such as those based on stem cells.

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Section: Approaches To Treatmentmentioning

confidence: 99%

Alpha One Antitrypsin Deficiency: From Gene to Treatment

Wood

Stockley

2007

Respiration

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“…The largest observational study analyzed data from 1,129 patients in the US AATD registry split into three groups “always receiving” (n=390), “partly receiving” (n=357), or “never receiving” (n=382) augmentation 33. Dosing was not standardized with only 51.3% being dosed weekly throughout the study.…”

Section: Resultsmentioning

confidence: 99%

“…Seventy-five patients had ≥1 exacerbation during the 18 months follow-up required prior to commencement of augmentation. Dosing regimens were not standardized with an average dose of 60.7±3.8 mg/kg/week (Table S1) different from other studies,33 and many patients had missing data. Fewer exacerbations were seen (1.2±1.6 vs 1.0±2.2 pre- vs posttreatment; P <0.01), an effect more marked in those exacerbating previously (2.0±1.6 vs 1.4±2.7; P <0.01).…”

Section: Resultsmentioning

confidence: 99%

Treatment of lung disease in alpha-1 antitrypsin deficiency: a systematic review

Edgar¹,

Patel²,

Bayliss³

et al. 2017

COPD

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BackgroundAlpha-1 antitrypsin deficiency (AATD) is a rare genetic condition predisposing individuals to chronic obstructive pulmonary disease (COPD). The treatment is generally extrapolated from COPD unrelated to AATD; however, most COPD trials exclude AATD patients; thus, this study sought to systematically review AATD-specific literature to assist evidence-based patient management.MethodsStandard review methodology was used with meta-analysis and narrative synthesis (PROSPERO-CRD42015019354). Eligible studies were those of any treatment used in severe AATD. Randomized controlled trials (RCTs) were the primary focus; however, case series and uncontrolled studies were eligible. All studies had ≥10 participants receiving treatment or usual care, with baseline and follow-up data (>3 months). Risk of bias was assessed appropriately according to study methodology.ResultsIn all, 7,296 studies were retrieved from searches; 52 trials with 5,632 participants met the inclusion criteria, of which 26 studies involved alpha-1 antitrypsin augmentation and 17 concerned surgical treatments (largely transplantation). Studies were grouped into four management themes: COPD medical, COPD surgical, AATD specific, and other treatments. Computed tomography (CT) density, forced expiratory volume in 1 s, diffusing capacity of the lungs for carbon monoxide, health status, and exacerbation rates were frequently used as outcomes. Meta-analyses were only possible for RCTs of intravenous augmentation, which slowed progression of emphysema measured by CT density change, 0.79 g/L/year versus placebo (P=0.002), and associated with a small increase in exacerbations 0.29/year (P=0.02). Mortality following lung transplant was comparable between AATD- and non-AATD-related COPD. Surgical reduction of lung volume demonstrated inferior outcomes compared with non-AATD-related emphysema.ConclusionIntravenous augmentation remains the only disease-specific therapy in AATD and there is evidence that this slows decline in emphysema determined by CT density. There is paucity of data around other treatments in AATD. Treatments for usual COPD may not be as efficacious in AATD, and further studies may be required for this disease group.

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“…Any discrepancies between the results of the assay and the quantitative test, as shown before, should prompt the physicians to ask for a plasma IEF or a more sophisticated molecular approach, such as allele-specific amplification, or sequence analysis [4]. Another, minor clinical application of the amplification-reverse hybridization assay kit, is to confirm a ZZ genotype in patients in whom, in spite of lacking precise AAT characterization, AAT replacement therapy has already been started [14]. …”

Section: Discussionmentioning

confidence: 99%

A Fast Amplification-Reverse Hybridization Assay Kit to Detect the Most Frequent Deficient Variants in the Alpha-1-Antitrypsin Gene

et al. 2002

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Background: There is worldwide growing awareness of alpha-1-antitrypsin deficiency (AATD), a major hereditary disorder in Caucasians. The gold standard for its laboratory diagnosis is thin-layer isoelectric focusing, which should be performed in reference laboratories. Objectives: The aim of this study was to check the characteristics of a commercially available amplification-reverse hybridization assay kit in detecting at a molecular level the alpha-1-antitrypsin (AAT) Z and S variants, i.e. the most frequent variants associated with AATD, by comparing its performance with DNA restriction fragment length polymorphism. Methods: We studied samples from 36 subjects enrolled in the Italian National Registry for Severe Alpha-1-antitrypsin Deficiency. Based on previous plasma isoelectric focusing typing, we selected samples with the following phenotypes: MM (9 samples), MS (9 samples), SZ (3 samples), MZ (11 samples), ZZ (3 samples), and a rare variant (1 sample). DNA was extracted by the standard method. The presence of the AAT Z and S gene variants was determined by the amplification-reverse hybridization test kit, following the manufacturer’s instructions, and by the restriction fragment length polymorphism technique, according to established procedures. Results: We found that the identification of the AAT Z and S gene variants obtained by the amplification-reverse hybridization test kit was completely in agreement with that obtained by the restriction fragment length polymorphism technique. Conclusions: We conclude that the test kit provides a fast, easy and unambiguous identification of Z and S alleles. Because of its transferability to routine laboratories, the test kit may be useful in identifying cases of severe AATD, thus resulting in increasing awareness of this rare disorder.

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Survival and FEV₁Decline in Individuals with Severe Deficiency of α₁-Antitrypsin

Cited by 385 publications

References 35 publications

Alpha One Antitrypsin Deficiency: From Gene to Treatment

Alpha One Antitrypsin Deficiency: From Gene to Treatment

Treatment of lung disease in alpha-1 antitrypsin deficiency: a systematic review

A Fast Amplification-Reverse Hybridization Assay Kit to Detect the Most Frequent Deficient Variants in the Alpha-1-Antitrypsin Gene

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Survival and FEV1Decline in Individuals with Severe Deficiency of α1-Antitrypsin

Cited by 385 publications

References 35 publications

Alpha One Antitrypsin Deficiency: From Gene to Treatment

Alpha One Antitrypsin Deficiency: From Gene to Treatment

Treatment of lung disease in alpha-1 antitrypsin deficiency: a systematic review

A Fast Amplification-Reverse Hybridization Assay Kit to Detect the Most Frequent Deficient Variants in the Alpha-1-Antitrypsin Gene

Contact Info

Product

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Survival and FEV₁Decline in Individuals with Severe Deficiency of α₁-Antitrypsin