600% Kurspotential YM Biosciences 911799

heute versteht man die ym-welt aber nicht so ganz
positive news und steil bergab
naja...wird schon werden

wenn man die Projekt nimo in USA u. Kanada aus Kostengründen einstellt...
...osciences-closes-nimotuzumab-trials-in-north-america-310511

man muss sich immer auf das konzentrieren was funktioniert, alles andere ist geldverschwendung. und alle neuen tests können niemals gut gehen.
hier werden wir noch viel spass haben...

viel zu wichtig, um das es unter dem Tisch fällt...?!

Ich glaubs einfach nicht, nur wegen dieser Meldung: www.minyanville.com/businessmarkets/...-asco/6/8/2011/id/35034

Ist doch alles noch gar nicht so weit entwickelt, um das es so einen Einfluss auf die Aktie hat, oder versteh ich da was falsch?

wann werden wir stoppen?

der Eibsche,bei diesem mieserablen Kurs :-(((

Global Biotech Investing - YM BioSciences Fokus liegt auf dem Medikament CYT387
09:54 05.10.11

Endingen (aktiencheck.de AG) - Die Experten von "Global Biotech Investing" empfehlen Anlegern, sich ein paar Stück der Aktie von YM BioSciences (YM BioSciences Aktie) abzugreifen.

Bei YM BioSciences liege der Fokus der Analysten aktuell auf dem Medikament CYT387 der Hämato-Onkologie. Auf der ASCO-Konferenz habe das Unternehmen zuletzt über den derzeitigen Entwicklungsstand der Arznei berichtet. Die Experten würden mit der kompletten Auswertung der Versuchsstudie gegen Ende des Jahres rechnen.

Nach Ansicht der Analysten von Bloom Burton habe der Kursrutsch der vergangenen Wochen nichts mit dem der CYT387-Studie zu tun, sondern sei auf die Turbulenzen am Gesamtmarkt zurückzuführen. Zudem sei der Kurs offenbar durch den direkten Vergleich von CYT387 mit dem Medikament Ruxolotinib von Incyte (INCYTE CORP Aktie) belastet worden. Beide Arzneien seien jedoch aktuell nicht vergleichbar, da Ruxolotinib ein Phase-III-Präparat sei, für das man gerade eine Zulassung bei der FDA eingereicht habe. Bis spätestens Anfang Dezember solle die Empfehlung eines FDA-Expertenpanels gefällt werden.

Nach Meinung der Experten von "Global Biotech Investing" sollten sich Zocker noch der Entscheidung ein paar Stücke der YM BioSciences-Aktie ins Depot holen. (Ausgabe 19 vom 04.10.2011) (05.10.2011/ac/a/a)


Offenlegung von möglichen Interessenskonflikten: Mögliche Interessenskonflikte können Sie auf der Site des Erstellers/ der Quelle der Analyse einsehen.

Quelle: Aktiencheck

wer ne Taxe für SK?

nur das Buran mit Helm und meiner McCulloch Kettensäge

momentmal,ich schmeiss mal meinen Hobel an und schaue mal nach wieviel Platz nach oben ist,ob genug für YM Bio ist      ....Vorsicht.....jodeldiejodeldieheyyyyyyyyyyyyyyyy

 Der Grund ist dann eher hier zu finden, positive Studien:

www.prnewswire.com/news-releases/...at-ash-2011-135468403.html

 

 

und morgen vielleicht schon wieder negativ?
Kopfschüttel...

genau, heute schon wieder südwärts - einfach nicht zu glauben!!!

@all

Der Eibsche ist'n Flachser

Gruss Buran

;o)

nicht sehr symphatisch.Bin nicht der grosse Rechner und schon garnicht der Mann von Welt,aber die 20 oben drauf und ich wäre mit knapp 1,60 vom Acker.

The Core Phase I/II study has completed enrollment of 166 myelofibrosis patients across six study sites. The Core study consists of nine 28-day treatment cycles where CYT387 is orally self-administered, primarily at dosages of 150 mg once-daily (QD), 300 mg QD or 150 mg twice-daily (BID). Patients who tolerate and benefit from the drug may continue to receive CYT387 beyond the Core study in an Extension phase. While data collection and analysis are ongoing, preliminary safety and efficacy results from this multicenter study are presented below.

Subject Characteristics
The majority of the 166 patients enrolled have Primary Myelofibrosis (65%); 22% have Post-Polycythemia vera and 14% have Post-Essential thrombocythemia. Other patient characteristics include :


DIPSS-Plus category: Int-1 - 11%; Int-2 - 61%; High - 28%
JAK2V617F positive: 76%
Red blood cell transfusion-dependent: 44%
Palpable splenomegaly >10 cm: 80%

The trial also enrolled patients who had received previous therapies, including other JAK inhibitors (12%) and IMiDs (9%).

Subject Disposition
The median follow-up time for patients in the Core study and Extension phase is 10.4 months (range: 0.8-25.6 months; ongoing). To date, 97% of patients who have completed the Core study have continued into the Extension phase. During the Core study, 32 patients (19%) have discontinued the study, five for possibly or probably related adverse events, for a current overall retention rate of 81%. The retention rate during the Extension phase is currently 79%.

Anemia Response
Of the 68 patients who were transfusion dependent at baseline, to date 54% have become transfusion independent for a minimum of 12 weeks. The median duration of the transfusion-free period has not yet been reached (range: 82-506 days, ongoing). More than 25% of subjects who were not receiving transfusions while on study experienced at least a 1 g/dL increase in hemoglobin lasting for more than eight weeks.

Of the 26 patients who were dosed at 300mg QD and were transfusion dependent at baseline, to date 65% have become transfusion independent for a minimum of 12 weeks.

Spleen Response
Of the 142 patients evaluable for spleen response, 31% achieved a response per IWG-MRT*. The median duration of spleen response has not yet been reached (range: 55 - 574 days, ongoing). The median time to spleen response was 15 days (range: 6 - 260 days, ongoing). To date, 49% of patients achieved more than a 50% maximal decrease in spleen size from baseline, with 87% achieving more than a 25% maximal decrease.

Of the 51 patients who were dosed at 300mg QD and were evaluable for spleen response, 33% achieved a response per IWG-MRT.

Eleven patients were evaluable for spleen response both by MRI and by palpation. The response rate was 64% by MRI (defined as a 35% decrease in spleen volume) and 45% by palpation (defined as a 50% decrease in spleen length). The median splenic decrease from baseline at three months was -41% by volume measured by MRI and -45% by length measured by palpation.

*International Working Group for Myelofibrosis Research and Treatment

Constitutional Symptoms Response
The majority of patients reporting constitutional symptoms at baseline demonstrated a Complete Resolution or Marked Improvement of their symptoms, including night sweats, pruritus and bone pain.

Safety Results
CYT387 is well tolerated in myelofibrosis patients for dosing periods up to and exceeding two years. Reported adverse effects include thrombocytopenia; transient, mild dizziness; mild peripheral neuropathy; and abnormalities in liver/pancreas-related laboratory tests. Treatment emergent anemia and neutropenia were rarely reported.

Poster presentation and YM conference call:
The updated results from the Phase I/II study will be presented in a poster session at the 53rd Annual Meeting of the American Society of Hematology. Poster #3849, entitled "Safety and Efficacy of CYT387, a JAK1 and JAK2 Inhibitor for the Treatment of Myelofibrosis", will be presented at Session #634, Myeloproliferative Syndromes: Poster III, being held on Monday, December 12th from 6:00-8:00pm PT in Hall GH of the San Diego Convention Center.

YM will also host a webcast meeting open to members of the investment community to discuss these results. This event will be held from 6:30-7:30am PT on Tuesday, December 13th in the Grand Ballroom of the Hotel Palomar, 1047 Fifth Avenue, San Diego. Access to the webcast will be available from YM's website at www.ymbiosciences.com or at www.newswire.ca. The event can also be heard by dialing in to (647) 427-7450 or toll-free at (888) 231-8191.

About CYT387:
CYT387 is an inhibitor of the kinase enzymes JAK1 and JAK2, which have been implicated in a family of hematological conditions known as myeloproliferative neoplasms, including myelofibrosis, and as well in numerous other disorders including indications in hematology, oncology and inflammatory diseases. Myelofibrosis is a chronic debilitating disease in which a patient's bone marrow is replaced by scar tissue and for which treatment options are limited or unsatisfactory.

Both the U.S. Food and Drug Administration (FDA) and the European Commission have designated CYT387 an Orphan Drug for the treatment of myelofibrosis.

YM BioSciences retains full global commercialization rights to CYT387.

About YM BioSciences
YM BioSciences Inc. is a drug development company advancing three products: CYT387, a small molecule, dual inhibitor of the JAK1/JAK2 kinases; nimotuzumab, an EGFR-targeting monoclonal antibody; and CYT997, a vascular disrupting agent (VDA).

CYT387 is an orally administered inhibitor of both the JAK1 and JAK2 kinases, which have been implicated in a number of immune cell disorders including myeloproliferative neoplasms and inflammatory diseases as well as certain cancers. CYT387 is currently in a 166 patient Phase I/II trial in myelofibrosis that has completed enrollment, as well as a 60 patient Phase II BID trial that is recruiting patients. Nimotuzumab is a humanized monoclonal antibody targeting EGFR with an enhanced side-effect profile over currently marketed EGFR-targeting antibodies. Nimotuzumab is being evaluated in numerous Phase II and III trials worldwide. CYT997 is an orally-available small molecule therapeutic with dual mechanisms of vascular disruption and cytotoxicity, and has completed a Phase II trial in glioblastoma multiforme. In addition to YM's three products, the Company has several preclinical research programs underway with candidates from its library of novel compounds identified through internal research conducted at YM BioSciences Australia.

This press release may contain forward-looking statements, which reflect the Company's current expectation regarding future events. These forward-looking statements involve risks and uncertainties that may cause actual results, events or developments to be materially different from any future results, events or developments expressed or implied by such forward-looking statements. Such factors include, but are not limited to, changing market conditions, the successful and timely completion of clinical studies, the establishment of corporate alliances, the impact of competitive products and pricing, new product development, uncertainties related to the regulatory approval process or the ability to obtain drug product in sufficient quantity or at standards acceptable to health regulatory authorities to complete clinical trials or to meet commercial demand; and other risks detailed from time to time in the Company's ongoing quarterly and annual reporting. Certain of the assumptions made in preparing forward-looking statements include but are not limited to the following: that CYT387, nimotuzumab and CYT997 will generate positive efficacy and safety data in ongoing and future clinical trials, and that YM and its various licensees will complete their respective clinical trials and disclose data within the timelines communicated in this release. Except as required by applicable securitieslaws, we undertake no obligation to publicly update or revise any forward-looking statements, whether as a result of new information, future events or otherwise.

SOURCE YM BioSciences Inc.


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da geht desöfteren immer mal wieder einer über Tradegate,bist Du das?

Gruss Buran

Über 13 % auf der anderen Seeseite bei gutem Volumen...

Ja hast  du gibt seit gestern Übernahme Gerüchte von ym Biosciences link ist http://www.finanzen.net/nachricht/aktien/...-Takeover-Chatter-1603454

 

Gruss

Jetzt hört man gerade nichts mehr neues hierzu, hat denn jemand Neuigkeiten?