Clazakizumab: Difference between revisions
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{{Short description|Chemical compound}} |
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| target = [[Interleukin 6|IL6]] |
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| CAS_number = 1236278-28-6 |
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| UNII_Ref = {{fdacite|correct|FDA}} |
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| UNII = 4S38Z8RA9O |
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| KEGG = D10312 |
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| C=6426 | H=9972 | N=1724 | O=2032 | S=42 |
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| synonyms = ALD518, BMS-945429 |
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'''ALD518''' an [[asialated]], humanized [[monoclonal antibody]] against [[interleukin-6]].<ref name=June2010/> It is an [[investigational drug]] for cancer and [[rheumatoid arthritis]] due to its anti-inflammatory properties. |
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'''Clazakizumab''' (formerly '''ALD518''' and '''BMS-945429'''), an [[investigational drug]], is an [[aglycosylated]], humanized rabbit [[monoclonal antibody]] against [[interleukin-6]].<ref name="Handbook">{{cite book|title=Handbook of Therapeutic Antibodies, Volume 2|date=2007|publisher=Wiley Blackwell|page=987|isbn=9783527329373|url=https://books.google.com/books?id=svHsBQAAQBAJ&q=Clazakizumab,+BMS-945429+ALD518&pg=PA987|access-date=January 23, 2017}}</ref> Clazakizumab was developed by [[Bristol Myers Squib]] and [[Alder Biopharmaceuticals]]. A preliminary randomized, double-blind, [[placebo]]-controlled, [[phase 2 clinical trial|phase 2]] dose-ranging study of clazakizumab in [[psoriatic arthritis]] patients, funded by the manufacturer, suggested that clazakizumab may be an effective treatment option for musculoskeletal aspects of [[psoriatic arthritis]]; however, the antibody lacked a [[dose-response effect]].<ref name="ArthRheum1">{{cite journal|vauthors=Mease PJ, Gottlieb AB|display-authors=etal|title=The efficacy and safety of clazakizumab, an anti-interleukin-6 monoclonal antibody, in a phase IIb study of adults with active psoriatic arthritis.|journal=Arthritis Rheumatol|date=September 2016|volume=68|issue=9|pages=2163–73|doi=10.1002/art.39700|pmid=27059799|s2cid=3644962}}</ref> |
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The relatively long half life of about 30 days should allow less frequent and subcutaneous injections.<ref name=XCFF>http://www.xconomy.com/seattle/2008/09/18/alder-sets-stage-for-showdown-with-roche-with-fast-follower-antibody-drug-strategy/</ref> |
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It is made using [[yeast]] cells rather than the standard [[Chinese hamster ovary cell]]s.<ref name=XCFF/> |
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==Clinical trials== |
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===Cancer=== |
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A phase I clinical trial showed ALD518 was well tolerated and could reverse fatigue in cancer patients.<ref>http://www.asco.org/ASCOv2/Meetings/Abstracts?&vmview=abst_detail_view&confID=65&abstractID=32916 "A phase I, pharmacokinetic (PK), and preliminary efficacy assessment of ALD518, a humanized anti-IL-6 antibody, in patients with advanced cancer." 2009</ref> |
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A phase II trial for advanced cancer is due to end in Oct 2009.<ref>http://www.boliven.com/clinical_trial/NCT00866970 Phase II: "Safety, Efficacy and Pharmacokinetics of ALD518 in Patients With Non-Small Cell Lung Cancer-Related Fatigue and Cachexia"</ref> Results due June 2010<ref>http://www.xconomy.com/seattle/2010/05/13/alder-seeks-to-treat-cancer-patients-in-a-radical-way-fighting-inflammation-not-tumors/?single_page=true </ref>. Results from 124 [[non-small cell lung cancer]] (NSCLC) patients were favourable (eg. 1/10th the weight loss).<ref name=June2010>{{cite web|url=http://www.empr.com/phase-2a-study-of-ald518-for-treatment-of-non-small-cell-lung-cancer-nsclc-symptoms/article/171887/ |title=Phase 2a study of ALD518 for treatment of non small cell lung cancer (NSCLC) symptoms |date=June 2010 }}</ref> |
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It may be trialled in a dual therapy with [[Tarceva]] owing to a likely synergy.<ref>http://www.nature.com/scibx/journal/v3/n35/full/scibx.2010.1056.html </ref> |
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===Rheumatoid arthritis=== |
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The Phase IIa trial for [[rheumatoid arthritis]]<ref>http://clinicaltrials.gov/ct2/show/NCT00867516</ref> has completed with promising results leading to a licencing deal allowing phase III trials.<ref>http://www.smartbrief.com/news/aanp/industryBW-detail.jsp?id=9279E59B-9E2A-4823-9476-17782B175A34 "Bristol-Myers Squibb and Alder Biopharmaceuticals Enter Global Agreement on Rheumatoid Arthritis Biologic" 10 Nov 2009</ref> The results are to be presented in June 2010 at the European League Against Rheumatism (EULAR) meeting in Rome.<ref>http://www.xconomy.com/seattle/2010/03/19/innovation-northwest-wrapup-alder-tekmira-acucela-other-emerging-little-biotechs/ </ref> |
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==References== |
==References== |
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{{ |
{{Reflist}} |
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{{Monoclonals for immune system}} |
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==External links== |
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{{Interleukin receptor modulators}} |
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*[http://www.alderbio.com/assets/File/2009_Wiesel_Partners_Healthcare_Conference.pdf ALD518 compared with tocilizumab(Actemra)] |
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[[Category:Drugs developed by Bristol Myers Squibb]] |
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{{pharma-stub}} |
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[[Category:Antibodies]] |
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[[Category:Experimental monoclonal antibodies]] |
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Latest revision as of 07:01, 2 December 2023
| Monoclonal antibody | |
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| Type | Whole antibody |
| Source | Humanized |
| Target | IL6 |
| Clinical data | |
| Other names | ALD518, BMS-945429 |
| Routes of administration | infusion |
| ATC code |
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| Legal status |
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| Chemical and physical data | |
| Formula | C6426H9972N1724O2032S42 |
| Molar mass | 145239.02 g·mol−1 |
Clazakizumab (formerly ALD518 and BMS-945429), an investigational drug, is an aglycosylated, humanized rabbit monoclonal antibody against interleukin-6.[1] Clazakizumab was developed by Bristol Myers Squib and Alder Biopharmaceuticals. A preliminary randomized, double-blind, placebo-controlled, phase 2 dose-ranging study of clazakizumab in psoriatic arthritis patients, funded by the manufacturer, suggested that clazakizumab may be an effective treatment option for musculoskeletal aspects of psoriatic arthritis; however, the antibody lacked a dose-response effect.[2]
See also
[edit]- Tocilizumab (Actemra) an anti-IL-6 receptor mAb
- Anti-IL-6, other anti-interleukin-6 agents
References
[edit]- ^ Handbook of Therapeutic Antibodies, Volume 2. Wiley Blackwell. 2007. p. 987. ISBN 9783527329373. Retrieved January 23, 2017.
- ^ Mease PJ, Gottlieb AB, et al. (September 2016). "The efficacy and safety of clazakizumab, an anti-interleukin-6 monoclonal antibody, in a phase IIb study of adults with active psoriatic arthritis". Arthritis Rheumatol. 68 (9): 2163–73. doi:10.1002/art.39700. PMID 27059799. S2CID 3644962.