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Home  /  Forum  /  Galapagos  /  Galapagos 2015: de inhoudelijke discussie

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Aandeel Galapagos AEX:GLPG.NL, BE0003818359

  • 27,120 24 apr 2024 17:35
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Galapagos 2015: de inhoudelijke discussie

3.351 Posts
Pagina: «« 1 ... 43 44 45 46 47 ... 168 »» | Laatste | Omlaag ↓
  1. [verwijderd] 16 september 2015 23:05
    www.wsj.com/articles/abbvie-hires-jp-...

    AbbVie Hires JP Morgan Banker As Chief Strategy Officer

    Henry Gosebruch to oversee deals and alliances, reporting to CEO Richard Gonzalez

    By PETER LOFTUS

    Sept. 16, 2015 4:30 p.m. ET
    Drug maker AbbVie Inc. is hiring a top investment banker from J.P. Morgan to a newly created senior strategy post, a sign that AbbVie plans to remain active on the deal front.
  2. NielsjeB 16 september 2015 23:18
    quote:

    BiostockAddict schreef op 16 september 2015 23:05:

    www.wsj.com/articles/abbvie-hires-jp-...

    AbbVie Hires JP Morgan Banker As Chief Strategy Officer

    Henry Gosebruch to oversee deals and alliances, reporting to CEO Richard Gonzalez

    By PETER LOFTUS

    Sept. 16, 2015 4:30 p.m. ET
    Drug maker AbbVie Inc. is hiring a top investment banker from J.P. Morgan to a newly created senior strategy post, a sign that AbbVie plans to remain active on the deal front.
    Precies op tijd! Snap sowieso niet waarom pharma-bedrijven die zakenbankiers niet vaker gewoon in dienst nemen. Dat moet toch een hoop geld schelen? Of zijn daar allerlei regels voor die dat belemmeren?
  6. [verwijderd] 19 september 2015 15:30
    Also Friday, RBC Capital Markets analyst Michael Yee wrote in a research note that he'd been hearing investor chatter about upcoming trial data from competing cystic-fibrosis players Galapagos (NASDAQ:GLPG) and ProQR Therapeutics (NASDAQ:PRQR), but he said he saw no big worry for Vertex on that score.
    "While Galapagos Phase I top-line and safety data is near term, this is only one part of a combo program and the hurdles are very high to develop and commercialize this and two more correctors, where all CF pts (cystic-fibrosis patients) will already be on Vertex drugs and unlikely to switch unless (Galapagos' drug is) much different," Yee wrote.
    Shares of lightly traded Galapagos were up 4.5% Friday afternoon, while ProQR stock was up 1.5%.

    news.investors.com/technology/091815-...
  10. Dr. Bob 20 september 2015 22:15
    quote:

    BiostockAddict schreef op 19 september 2015 15:26:

    @BiotechRadar: AbbVie's comments on $GLPG JAK1 inhibitor program at Morgan Stanley Global Healthcare Conference yesterday #phase3 - t.co/yscvpohy0R
    Transcript:
    "You probably are going to be hearing more about our internal JAK1-inhibitor ABT-494 as we work through how we are going to proceed with our portfolio of selective JAK1 inhibitors, Galapagos and 494, we are certainly looking to initiate a phase III in rheumatoid arthritis before the end of this year."
  12. NielsjeB 21 september 2015 23:57
    Poster PA2129 die wordt gepresenteerd op de ERS 2015 (28 september, 10:45-12:45):

    Pharmacological profile and efficacy of GLPG1690, a novel ATX inhibitor for COPD treatment

    Roland Blanque, Nicolas Desroy, Sonia Dupont, Céline Cottereaux, Alain Monjardet, Emanuelle Wakselman, Wendy Laenen, Vince Russell, Ellen Van der Aar, Reginald Brys, Bertrand Heckmann

    Introduction
    Autotaxin (ATX), a secreted lysophospholipase, plays a central role in the production of the bioactive lipid lysophosphatidic acid (LPA). LPA signals through multiple LPA receptors to control a range of cell activities (migration, contraction, survival…). Recently, a role for the ATX/LPA axis in asthma and fibrosis were reported, suggesting involvement in additional lung diseases.
    Aims & objectives
    To characterize the pharmacological profile of GLPG1690, a novel ATX inhibitor, as well as its efficacy in COPD.
    Methods
    Biochemical potency was assessed using human and mouse recombinant ATX. Ex vivo potency was determined in plasma by measuring LPA levels (LC-MS) after incubation with GLPG1690. Plasma LPA levels of GLPG1690-treated animals was used as pharmacodynamic marker. Inflammatory cell counts in bronchoalveolar lavage fluid (BALF) were used as a measure for efficacy in a mouse 11-day tobacco smoke (TS) model for COPD.
    Results
    GLPG1690 was shown to be a potent inhibitor of mouse and human ATX (IC50: 100-500 nM range). Similar potency was observed ex vivo in human and rodent plasma. In a therapeutic mouse COPD model, GLPG1690 (3, 10 and 30 mg/kg b.i.d., p.o.), dose-dependently reduced inflammatory cell counts in the BALF to a similar extent as roflumilast (5 mg/kg q.d., p.o.). In GLPG1690-treated mice, an inverse relationship was shown between LPA and GLPG1690 plasma levels.
    Conclusion
    GLPG1690, a potent and selective ATX inhibitor, displays a strong overall developability profile, supporting the progression towards First-in-Human studies. For the first time, efficacy of an ATX inhibitor was shown in a model for COPD, pointing to a novel therapeutic area for this target.

    www.erscongress.org/images/congress20...
    www.erscongress.org/programme-2015/ac...
  13. NielsjeB 21 september 2015 23:59
    Abstract OA484 die wordt gepresenteerd op de ERS 2015 (27 september, 11:15):

    Favorable human safety, pharmacokinetics and pharmacodynamics of the autotaxin inhibitor GLPG1690, a potential new treatment in COPD

    Ellen Van der Aar, Liesbeth Fagard, Julie Desrivot, Sonia Dupont, Bertrand Heckmann, Roland Blanque, Lien Gheyle, Jovica Ralic, Frédéric Vanhoutte

    Introduction
    Autotaxin (ATX) is a secreted enzyme with lysophospholipase D activity responsible for the production of the bioactive lipid lysophosphatidic acid (LPA). LPA acts through several LPA receptors which promote among others cell proliferation, survival and muscle contraction. Recently, a role for the ATX/LPA axis was reported in several lung diseases.
    We identified GLPG1690 as a potent and selective inhibitor of ATX. It has good ADME and pharmacokinetic properties and showed dose-related effects in a mouse tobacco smoke COPD model.
    Aim and objectives
    To evaluate the safety, tolerability, pharmacokinetics and pharmacodynamics (PD) of GLPG1690 in healthy subjects.
    Methods
    GLPG1690 was administered as single oral doses (20 up to 1500 mg) or multiple doses (up to 1000 mg for 14 days). Each dose level was evaluated in panels of 8 male healthy subjects, 6 receiving GLPG1690 and 2 placebo. PD was assessed by the measurement of LPA18:2 levels in plasma via LC-MS.
    Results
    GLPG1690 was safe and well tolerated up to a single oral dose of 1500 mg and up to 1000 mg q.d. for 14 days, with no adverse effects on ECGs, vital signs or laboratory parameters. The compound showed good oral bioavailability with a half-life of 5 h and a dose-proportional increase in exposure. GLPG1690 showed concentration-dependent reduction of plasma LPA18:2 levels with a maximum of approximately 90%. At steady state, continuous reduction of LPA18:2 levels of >60% was observed from 0 to 24 h.
    Conclusion
    These data in healthy subjects and the preclinical data generated encourage Galapagos to explore a Phase 2 study design in pulmonary disease.

    www.erscongress.org/images/congress20...
    www.erscongress.org/programme-2015/ac...
  15. Renno54 22 september 2015 06:42


    Galapagos 'perfect fit' voor AbbVie

    Gepubliceerd op 21 sep 2015 om 17:56 | Views: 4.824 | Onderwerpen: biotechnologie

    Artikel

    Reacties

    Gerelateerde instrumenten

    Galapagos 21 sep

    58,32 0,00 (+9,19%)


    AMSTERDAM (AFN/BLOOMBERG) - De Amerikaanse farmaceut AbbVie lijkt naar kleinere overnames in de sector. Dat zei de financieel topman van het bedrijf vrijdag volgens analisten van Bryan Garnier, tijdens een beleggersbijeenkomst. Het bedrijf ziet daarbij Galapagos als een 'perfect fit', zo zou de bestuurder hebben aangegeven.

    Galapagos en AbbVie zijn al samenwerkingspartners. AbbVie moet binnenkort een besluit geven over het nemen van een licentie op het Galapagos-middel filgotinib. De piekverkopen van dat product worden geschat op 2 miljard euro.

    Galapagos sloot maandag 9,2 procent hoger op 58,32 euro.
  16. pardon 22 september 2015 08:00
    Galapagos: positieve resultaten met GLPG1690
    Gepubliceerd op 22 sep 2015 om 07:58 | | Onderwerpen: biotechnologie
    Galapagos 21 sep
    58,32 0,00 (0,00%)

    MECHELEN (AFN) - Galapagos heeft positieve fase 1-testresultaten behaald met het middel GLPG1690 tegen longziekten. Dat maakte het Belgische biotechnologiebedrijf dinsdag bekend.

    De resultaten worden gepresteerd op het jaarlijkse longziektencongres van de European Respiratory Society in Amsterdam. Galapagos toont als eerste de werkzaamheid aan van een autotaxin-remmer bij de longziekten COPD en IPF. GLPG1690 is een sterke remmer van autotaxin in muizen en mensen
  18. Maycon 22 september 2015 09:08
    quote:

    NielsjeB schreef op 21 september 2015 23:59:

    Abstract OA484 die wordt gepresenteerd op de ERS 2015 (27 september, 11:15):

    Favorable human safety, pharmacokinetics and pharmacodynamics of the autotaxin inhibitor GLPG1690, a potential new treatment in COPD

    Ellen Van der Aar, Liesbeth Fagard, Julie Desrivot, Sonia Dupont, Bertrand Heckmann, Roland Blanque, Lien Gheyle, Jovica Ralic, Frédéric Vanhoutte

    Introduction
    Autotaxin (ATX) is a secreted enzyme with lysophospholipase D activity responsible for the production of the bioactive lipid lysophosphatidic acid (LPA). LPA acts through several LPA receptors which promote among others cell proliferation, survival and muscle contraction. Recently, a role for the ATX/LPA axis was reported in several lung diseases.
    We identified GLPG1690 as a potent and selective inhibitor of ATX. It has good ADME and pharmacokinetic properties and showed dose-related effects in a mouse tobacco smoke COPD model.
    Aim and objectives
    To evaluate the safety, tolerability, pharmacokinetics and pharmacodynamics (PD) of GLPG1690 in healthy subjects.
    Methods
    GLPG1690 was administered as single oral doses (20 up to 1500 mg) or multiple doses (up to 1000 mg for 14 days). Each dose level was evaluated in panels of 8 male healthy subjects, 6 receiving GLPG1690 and 2 placebo. PD was assessed by the measurement of LPA18:2 levels in plasma via LC-MS.
    Results
    GLPG1690 was safe and well tolerated up to a single oral dose of 1500 mg and up to 1000 mg q.d. for 14 days, with no adverse effects on ECGs, vital signs or laboratory parameters. The compound showed good oral bioavailability with a half-life of 5 h and a dose-proportional increase in exposure. GLPG1690 showed concentration-dependent reduction of plasma LPA18:2 levels with a maximum of approximately 90%. At steady state, continuous reduction of LPA18:2 levels of >60% was observed from 0 to 24 h.
    Conclusion
    These data in healthy subjects and the preclinical data generated encourage Galapagos to explore a Phase 2 study design in pulmonary disease.

    www.erscongress.org/images/congress20...
    www.erscongress.org/programme-2015/ac...
    Abstract OA484 ???
  19. NielsjeB 22 september 2015 09:57
    quote:

    winx08 schreef op 22 september 2015 08:45:

    [...]

    volgens mij heb je pesoonlijk een PB getriggered :-)
    Keep up the good work.

    Haha, mijn eerste gedachte, maar dat lijkt me iets teveel eer. Ik was sowieso niet van plan om erop te handelen. Het is goed nieuws, maar voorlopig niet meer dan dat.
3.351 Posts
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