Enzyme replacement therapy for Anderson-Fabry disease: A complementary overview of a Cochrane publication through a linear regression and a pooled analysis of proportions from cohort studies

Dib, Regina El; Gomaa, Huda; Ortíz, Alberto; Politei, Juan; Kapoor, Anil; Barreto, Fellype Carvalho

doi:10.1371/journal.pone.0173358

Cited by 74 publications

(64 citation statements)

References 96 publications

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“…38,39 In addition, ERT (agalsidase beta) led to significant reductions in the clinically significant composite renal, cardiac, and neurologic endpoint (-61%, P = 0.034, for the "per--protocol" population). 40,41 Numerous clinical observations also indicated that the clinical effects depend on the stage of the disease in which ERT was initiated. The use of ERT in patients at a younger age, with less severe organ damage, without irreversible complications, or without previous serious cardiovascular events, resulted in more beneficial clinical effects.…”

Section: Diagnosis Of Fabry Diseasementioning

confidence: 99%

“…Special indications for diagnostic testing for Fabry disease Chronic kidney disease, proteinuria, or albuminuria of unknown origin Unexplained left ventricular hypertrophic cardiomyopathy Transient ischemic attack or stroke in young people White matter lesions with an unclear cause Unexplained neuropathy of thin nerve fibers Angiokeratoma or cornea verticillataFamily history of Fabry disease (indication for active family screening of patients with diagnosed disease; inheritance related to the X chromosome) Effect of enzyme replacement therapy on clinical parameters in patients with Fabry disease (based on Germain et al,38 Germain et al,39 Banikazemi et al,40 and El Dib et al)41 …”

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confidence: 99%

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Enzyme replacement therapy in Fabry disease in Poland – position statement

Nowicki

Bazan-Socha

Błażejewska-Hyżorek

et al. 2019

Polish Archives of Internal Medicine

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associated with thin nerve fiber involvement occur, such as impaired perspiration (hypohidrosis, anhidrosis), abdominal pain, and diarrhea. Characteristic symptoms of the classic form also include angiokeratoma-type cutaneous lesions and corneal opacities (cornea verticillata). 1 Even in childhood, clinically silent proteinuric chronic kidney disease (CKD) may occur with microalbuminuria or glomerulosclerosis. Multiorgan symptoms of the classic form of FD usually appear in young adults and may include CKD, left ventricular hypertrophy, myocardial fibrosis, arrhythmias and conduction abnormalities, transient ischemic attack, and stroke. People with late-onset FD typically experience cardiac symptoms, stroke, or CKD in the fourth or fifth decade of life. 1 The classic form is an early-onset multisystem disease that usually presents with cornea verticillata and angiokeratomas. In contrast, the nonclassic form has a later onset and usually affects a single organ, most often the heart; angiokeratomas or cornea verticillata is rare. The progression of cellular and organ changes is observed in the course of FD. Metabolite accumulation begins as early as in the fetal period, leading to the involvement of numerous tissues and severe organ damage (FIguRE 1). 4 The life

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Section: Diagnosis Of Fabry Diseasementioning

confidence: 99%

mentioning

confidence: 99%

Enzyme replacement therapy in Fabry disease in Poland – position statement

Nowicki

Bazan-Socha

Błażejewska-Hyżorek

et al. 2019

Polish Archives of Internal Medicine

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“…53 However, recent reviews reported only a small benefit of the use of ERT. 66,80 One mechanism suspected to play a role in curbing ERT efficacy is the formation of ADAs against infused enzymes, which is a major focus of this review.…”

Section: Fd-specific Treatmentmentioning

confidence: 99%

Effects of Enzyme Replacement Therapy and Antidrug Antibodies in Patients with Fabry Disease

Lenders

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2018

JASN

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FOS, Fabry outcome survey; 95% CI, 95% confidence interval; LRI, low renal impairment; HRI, high renal impairment; mGFR, measured glomerular filtration rate; OR, odds ratio. 62 95% CI, 95% confidence interval; FOS, Fabry outcome survey; LRI, low renal impairment; HRI, high renal impairment; LVMI, left ventricular mass index; LVM, left ventricular mass; MWT, mean wall thickness; LVH, left ventricular hypertrophy; IVST, interventricular septum thickness; RWT, relative wall thickness; LVWT, left ventricular wall thickness.

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“…Left ventricular (LV) myocardial hypertrophy (LVMH) and cardiac fibrosis have been suggested as risk factors for arrhythmias and sudden death (Krämer et al, ). Currently, it is widely accepted that enzyme replacement therapy (ERT) provides benefits in terms of cardiac hypertrophy and renal disease, at least when initiated in the early stage of the disease (El Dib et al, ). Migalastat (or 1‐deoxygalactonojirimycin hydrochloride) has first been described as a competitive inhibitor of the α‐Gal A.…”

Section: Introductionmentioning

confidence: 99%

Strong increase of leukocyte apha‐galactosidase A activity in two male patients with Fabry disease following oral chaperone therapy

Lamari

Mauhin

Koraichi³

et al. 2019

Molec Gen & Gen Med

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Background Fabry disease (OMIM 301500) is an X‐linked disorder caused by alpha‐galactosidase A (α‐Gal A) deficiency. The administration of a pharmacologic chaperone (migalastat) in Fabry patients with amenable mutations has been reported to improve or stabilize organ damages and reduce lyso‐Gb3 plasma level. An increase of α‐Gal A activity has been observed in vitro in cells expressing amenable GLA mutations when incubated with migalastat. The impact of the drug on α‐Gal A in vivo activity has been poorly studied. Methods We conducted a retrospective analysis of two unrelated male Fabry patients with p.Asn215Ser (p.N215S) variant. Results We report the important increase of α‐Gal A activity in blood leukocytes reaching normal ranges of activity after about 1 year of treatment with migalastat. Cardiac parameters improved or stabilized with the treatment. Conclusion We confirm in vivo the effects of migalastat that have been observed in N215S carriers in vitro. The increase of α‐Gal A activity may be the strongest marker for biochemical efficacy. The normalization of enzyme activity could become the new therapeutic target to achieve.

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Enzyme replacement therapy for Anderson-Fabry disease: A complementary overview of a Cochrane publication through a linear regression and a pooled analysis of proportions from cohort studies

Cited by 74 publications

References 96 publications

Enzyme replacement therapy in Fabry disease in Poland – position statement

Enzyme replacement therapy in Fabry disease in Poland – position statement

Effects of Enzyme Replacement Therapy and Antidrug Antibodies in Patients with Fabry Disease

Strong increase of leukocyte apha‐galactosidase A activity in two male patients with Fabry disease following oral chaperone therapy

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