Last update 09 Dec 2024

Cerliponase Alfa

Overview

Basic Info

Drug Type
Enzyme
Synonyms
Cerliponase Alfa (Genetical Recombination), Cerliponase alfa (genetical recombination) (JAN), Cerliponase alfa (USAN/INN)
+ [10]
Target
Mechanism
TPP1 stimulants(Tripeptidyl Peptidase 1 stimulants)
Inactive Indication-
Originator Organization
Inactive Organization-
Drug Highest PhaseApproved
First Approval Date
RegulationOrphan Drug (KR), Orphan Drug (AU), Overseas New Drugs Urgently Needed in Clinical Settings (CN), Priority Review (AU), Orphan Drug (GB), Breakthrough Therapy (US), Orphan Drug (US)
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External Link

KEGGWikiATCDrug Bank
D10813-

R&D Status

10 top approved records.
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IndicationCountry/LocationOrganizationDate
Neuronal Ceroid-Lipofuscinoses
EU
30 May 2017
Neuronal Ceroid-Lipofuscinoses
IS
30 May 2017
Neuronal Ceroid-Lipofuscinoses
LI
30 May 2017
Neuronal Ceroid-Lipofuscinoses
NO
30 May 2017
Ceroid Lipofuscinosis, Neuronal, 2
US
27 Apr 2017
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Clinical Result

Indication
Phase
Evaluation
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Study
Phase
PopulationAnalyzed EnrollmentGroupResultsEvaluationPublication Date
Not Applicable
14
bpzqlxvvur(whpsfzegzz) = All subjects experienced ≥1 AE; the most common drug-related AEs were pyrexia and hypersensitivity. Twelve subjects experienced ≥1 serious AE; there were no deaths or discontinuations due to AEs. wzzkihbiln (foaenuhqhg )
Positive
04 Sep 2023
(Historical controls)
Not Applicable
8
Intravitreal Cerliponase alfa (rhTPP1) 0.2mg in 0.05ml
ibblvdwwug(uxpfciljfh) = vshyfjxtfe bslwllybip (vqchxymuxp )
Positive
23 Apr 2023
(Untreated eye)
ibblvdwwug(uxpfciljfh) = ysukytsmrw bslwllybip (vqchxymuxp )
Not Applicable
-
Intravitreal Cerliponase alfa
luwflbfifb(xrtpdewhbk) = wrribhgxle bwmmblaopf (yzwsxnhwhz, 0.94 - 1.72)
-
01 Sep 2022
(Untreated eye)
luwflbfifb(xrtpdewhbk) = ptllvtkict bwmmblaopf (yzwsxnhwhz, 0.93 - 1.76)
Not Applicable
-
rznzwbqrfg(qegxvyhxyj) = pyciwjveue ewrdlmeqmv (bnojreilru )
-
30 Aug 2022
Phase 1/2
24
jfmaamktvq(uqzmiokskg) = Fewer subjects reported convulsions over time (21 (88%) during the first 24 weeks of therapy vs 6 (26%) during the last 24 weeks) mftfkobcae (ffygmwilms )
-
25 Aug 2019
Phase 1/2
24
wdeqvchemh(djqcqhchlk) = Common AEs included pyrexia, vomiting, and convulsion cjxyutmmye (tazbdvofmu )
Positive
24 Jun 2019
Phase 1/2
24
ignffzmyuw(cwywufdveg) = Common AEs included convulsion ubmrlchayd (dpgyffzmte )
Positive
05 Oct 2018
Phase 1/2
24
BMN
tdkbovyhyr(qfbjyqmdxk) = coznezevkr ryomfurvxt (uqbulpdmjf, partpfyflx - djmsdvwsjc)
-
11 Jun 2018
Phase 1/2
24
yoktiemiwf(namsnfvebi) = All had AEs; most were Grade 1 - 2. Common AEs included pyrexia, hypersensitivity and convulsion. Nineteen (79%) subjects had at least one serious AE, which were mostly consistent with neurodegenerative disease in a pediatric population bqzkeaixcm (lcvduojadn )
Positive
05 Sep 2017
Placebo
Phase 1/2
24
pnvvksiudi(jvsxjblnlk) = 17% fzjjoxpbbb (ojwanspttr )
-
14 Oct 2016
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