DK2865751T3 - Stabiliseret alpha-galactosidase og anvendelser deraf - Google Patents
Stabiliseret alpha-galactosidase og anvendelser deraf Download PDFInfo
- Publication number
- DK2865751T3 DK2865751T3 DK14195875.1T DK14195875T DK2865751T3 DK 2865751 T3 DK2865751 T3 DK 2865751T3 DK 14195875 T DK14195875 T DK 14195875T DK 2865751 T3 DK2865751 T3 DK 2865751T3
- Authority
- DK
- Denmark
- Prior art keywords
- galactosidase
- gly
- leu
- val
- ala
- Prior art date
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Claims (17)
- Stabiliseret alpha-qalactosidase og anvendelser deraf1. Multimerisk proteinstruktur, der omfatter mindst to a-galactosidasemonomerer, der er kovalent bundet til hinanden via en linker-del, hvor linker-delen ikke er til stede i nativ α-galactosidase, hvilken multimerisk proteinstruktur er beregnet til anvendelse til behandling af Fabry-sygdom.
- 2. Multimerisk proteinstruktur til anvendelse ifølge krav 1, hvor den multimeriske proteinstruktur har en egenskab, der er udvalgt fra gruppen bestående af: (a) en α-galactosidaseaktivitet efter udsættelse af den multimeriske proteinstruktur for humane plasmaforhold i en time, der er mindst 10 % højere end en aktivitet for en nativ α-galactosidase efter udsættelse af den native α-galactosidase for humane plasmaforhold i en time; (b) en α-galactosidaseaktivitet, der falder efter udsættelse af den multimeriske proteinstruktur for humane plasmaforhold i en time ved en procentsats, der er mindst 10 % mindre end procentsatsen, ved hvilken en aktivitet for den native α-galactosidase falder efter udsættelse af den native α-galactosidase for de humane plasmaforhold i en time; (c) en α-galactosidaseaktivitet, der forbliver i alt væsentligt uændret efter udsættelse af den multimeriske proteinstruktur for humane plasmaforhold i en time; (d) en α-galactosidaseaktivitet efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold i en uge, der er mindst 10 % højere end en aktivitet for den native α-galactosidase efter udsættelse af den native α-galactosidase for de lysosomale forhold i en uge; (e) en α-galactosidaseaktivitet, der falder efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold i en dag ved en procentsats, der er mindst 10 % mindre end procentsatsen, ved hvilken en aktivitet for den native α-galactosidase falder efter udsættelse af den native α-galactosidase for lysosomale forhold i en dag; (f) en α-galactosidaseaktivitet, der forbliver i alt væsentligt uændret efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold i en dag; (g) en α-galactosidaseaktivitet umiddelbart efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold, der er mindst 10 % højere end en aktivitet for nativ α-galactosidase umiddelbart efter udsættelse af den native α-galactosidase for lysosomale forhold; (h) en α-galactosidaseaktivitet umiddelbart efter udsættelse af den multimeriske proteinstruktur for en vandig opløsning, der har et pH på 7 og en temperatur på 37 °C, der er mindst 10 % højere end en aktivitet for nativ α-galactosidase umiddelbart efter udsættelse af den native α-galactosidase for den vandige opløsning, der har et pH på 7 og en temperatur på 37 °C; og (i) en halveringstid i kredsløbet i et fysiologisk system, der er højere end en halveringstid i kredsløbet for den native α-galactosidase.
- 3. Multimerisk proteinstruktur til anvendelse ifølge krav 2, hvor a-galactosidaseaktiviteten for den multimeriske proteinstruktur, der forbliver i alt væsentligt uændret efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold i en dag, endvidere forbliver i alt væsentligt uændret efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold i en uge.
- 4. Multimerisk proteinstruktur til anvendelse ifølge et hvilket som helst af kravene 1 til 3, hvor den multimeriske proteinstruktur omfatter to α-galactosidasemonomerer, hvilken proteinstruktur er en dimerisk proteinstruktur.
- 5. Multimerisk proteinstruktur til anvendelse ifølge et hvilket som helst af kravene 1 til 4, hvor α-galactosidasen er en α-galactosidase genereret ved rekombinant teknologi.
- 6. Multimerisk proteinstruktur til anvendelse ifølge et hvilket som helst af kravene 1 til 5, hvor α-galactosidasen er en human α-galactosidase, der er udvalgt fra gruppen bestående af agalsidase alpha og agalsidase beta.
- 7. Multimerisk proteinstruktur til anvendelse ifølge et hvilket som helst af kravene 1 til 5, hvor α-galactosidasen har en aminosyresekvens, der er udvalgt fra gruppen bestående af SEQ ID NO: 1, SEQ ID NO: 2 og SEQ ID NO: 3.
- 8. Multimerisk proteinstruktur til anvendelse ifølge et hvilket som helst af kravene 1 til 7, hvor linker-delen er mindst 20 atomer lang.
- 9. Multimerisk proteinstruktur til anvendelse ifølge et hvilket som helst af kravene 1 til 8, hvor linker-delen omfatter en poly(alkylenglycol).
- 10. Multimeriske proteinstrukturer til anvendelse ifølge et hvilket som helst af kravene 1 til 8, hvor linker-delen har en almen formel: -Xi-(CRi R2-CR3R4-Y)n-X2- hvor hver af Xi og X2 er en funktionel gruppe, der danner en kovalent binding med mindst én a-galactosidasemonomer; Y er O, S eller NR5; n er et heltal fra 1 til 200; og hver af Ri, R2, R3, Rt og Rs uafhængigt er udvalgt fra gruppen bestående af hydrogen, alkyl, cycloalkyl, alkenyl, alkynyl, alkoxy, hydroxy, oxo, thiol og thioalkoxy.
- 11. Multimerisk proteinstruktur til anvendelse ifølge krav 10, hvor n er mindst 25.
- 12. Multimerisk proteinstruktur til anvendelse ifølge krav 10, hvor den multimeriske proteinstruktur omfatter to α-galactosidasemonomerer, hvor proteinstrukturen er en dimerisk proteinstruktur, hvor α-galactosidasen har en aminosyresekvens, der er udvalgt fra gruppen bestående af SEQ ID NO: 1, SEQ ID NO: 2 og SEQ ID NO: 3, hver af de funktionelle grupper danner en amidbinding med en α-galactosidasemonomer, og n er et heltal fra 40 til 70.
- 13. Multimeriske proteinstruktur til anvendelse ifølge krav 7, hvor den multimeriske proteinstruktur omfatter to a-galactosidasemonomerer, hvilken proteinstruktur er en dimerisk proteinstruktur, hvor linker-delen har formlen:hvor en molekylvægt af polyethylenglycolen i linker-delen er 2 kDa, og de terminale grupper af linker-delen hver danner en amidbinding med en a-galactosidasemonomer.
- 14. Farmaceutisk sammensætning til anvendelse til behandling af Fabry-sygdom ved parenteral administration, hvilken sammensætning omfatter den multimeriske proteinstruktur ifølge et hvilket som helst af kravene 1 til 13 og en farmaceutisk acceptabel bærer.
- 15. Sammensætning til anvendelse ifølge krav 14, hvor den parenterale administration er intravenøs infusion.
- 16. Sammensætning til anvendelse ifølge krav 14 eller 15, hvor en koncentration af den multimeriske proteinstruktur er 2 mg/ml.
- 17. Farmaceutisk sammensætning til anvendelse til behandling af Fabry-sygdom ved parenteral administration, hvilken sammensætning omfatter: (i) en multimerisk proteinstruktur, der omfatter mindst to a-galactosidasemonomerer, der er kovalent bundet til hinanden via en linker-del; og (ii) en farmaceutisk acceptable bærer, hvor den multimeriske proteinstruktur har en egenskab, der er udvalgt fra gruppen bestående af: (a) en α-galactosidaseaktivitet efter udsættelse af den multimeriske proteinstruktur for humane plasmaforhold i en time, der er mindst 10 % højere end en aktivitet for nativ α-galactosidase efter udsættelse af den native α-galactosidase for humane plasmaforhold i en time; (b) en α-galactosidaseaktivitet, der falder efter udsættelse af den multimeriske proteinstruktur for humane plasmaforhold i en time ved en procentsats, der er mindst 10 % mindre end procentsatsen, ved hvilken en aktivitet for den native α-galactosidase falder efter udsættelse af den native α-galactosidase for humane plasmaforhold i en time; (c) en α-galactosidaseaktivitet, der forbliver i alt væsentligt uændret efter udsættelse af den multimeriske proteinstruktur for humane plasmaforhold i en time; (d) en α-galactosidaseaktivitet efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold i en uge, der er mindst 10 % højere end en aktivitet for nativ a-galactosidase efter udsættelse af den native α-galactosidase for lysosomale forhold i en uge; (e) en α-galactosidaseaktivitet, der falder efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold i en dag ved en procentsats, der er mindst 10 % mindre end procentsatsen, ved hvilken en aktivitet for den native α-galactosidase falder efter udsættelse af den native α-galactosidase for lysosomale forhold i en dag; (f) en α-galactosidaseaktivitet, der forbliver i alt væsentligt uændret efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold i en dag; (g) en α-galactosidaseaktivitet, umiddelbart efter udsættelse af den multimeriske proteinstruktur for lysosomale forhold, der er mindst 10 % højere end en aktivitet for native α-galactosidase umiddelbart efter udsættelse af den native α-galactosidase for lysosomale forhold; (h) en α-galactosidaseaktivitet, umiddelbart efter udsættelse af den multimeriske proteinstruktur for en vandig opløsning, der har et pH på 7 og en temperatur på 37 °C, der er mindst 10 % højere end en aktivitet for nativ α-galactosidase umiddelbart efter udsættelse af den native α-galactosidase for den vandige opløsning, der har et pH på 7 og en temperatur på 37 °C; og (i) en halveringstid i kredsløbet i et fysiologisk system, der er mindst 20 % højere end halveringstiden i kredsløbet for den native α-galactosidase.
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US30948710P | 2010-03-02 | 2010-03-02 | |
PCT/IL2010/000956 WO2011061736A1 (en) | 2009-11-17 | 2010-11-17 | Alkaline alpha galactosidase for the treatment of fabry disease |
US201161434499P | 2011-01-20 | 2011-01-20 | |
US201161434503P | 2011-01-20 | 2011-01-20 | |
EP11712340.6A EP2542675B1 (en) | 2010-03-02 | 2011-03-02 | Stabilized alpha-galactosidase and uses thereof |
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US9194011B2 (en) | 2009-11-17 | 2015-11-24 | Protalix Ltd. | Stabilized alpha-galactosidase and uses thereof |
JP5758920B2 (ja) * | 2010-03-02 | 2015-08-05 | プロタリクス リミテッド | 安定化α−ガラクトシダーゼおよびその使用 |
EP2665814B1 (en) * | 2011-01-20 | 2017-05-17 | Protalix Ltd. | Nucleic acid construct for expression of alpha-galactosidase in plants and plant cells |
TWI793159B (zh) * | 2013-10-23 | 2023-02-21 | 美商健臻公司 | 重組醣蛋白及其用途 |
PL3237621T3 (pl) * | 2014-12-22 | 2023-10-30 | Codexis, Inc. | Warianty ludzkiej alfa-galaktozydazy |
WO2016116966A1 (en) * | 2015-01-22 | 2016-07-28 | Jcr Pharmaceuticals Co., Ltd. | Method for purification of recombinant human alpha-galactosidase a from material containing contaminant host cell proteins |
PL3271453T3 (pl) | 2015-03-17 | 2022-01-17 | eleva GmbH | Glikozylowane białka lizosomowe, sposób wytwarzania i zastosowania |
GB201508025D0 (en) | 2015-05-11 | 2015-06-24 | Ucl Business Plc | Fabry disease gene therapy |
BR112019013920A2 (pt) * | 2017-01-05 | 2020-02-04 | Protalix Ltd | método para tratar doença de fabry, e, forma unitária de dosagem. |
JP7171560B2 (ja) * | 2017-06-07 | 2022-11-15 | 天野エンザイム株式会社 | ラクターゼ原末及びラクターゼ製剤 |
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