Sagt die FDA doch ja ....
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Und die dazu befähigste Person ist Genta's CEO Raymond R. Warrel. Der Trustee wird also die Direktoren sicherlich befragen, wie es um den potentiellen Wert der Assets, als der in der Entwicklung befindlichen Medikamente steht.
Als Aktionär haben wir ja schon mehrfach auf den potentiellen (Markt)-Wert funktionierender Krebsmedikamente hingewiesen.
http://www.cozen.com/
Interessant ist, welche Gebiete der Expertise sie aufweisen:
Business/Corporate
Government & Regulatory
Insurance
Intellectual Property
Labor & Employment
Litigation
Real Estate
Subrogation & Recovery
Services
With Miller Coffey Tate LLP's emphasis on personal service to our clients and their individual business needs in mind, our services include:
•Auditing, Review and Compilation
•Bankruptcy, Litigation Support and Fraud Investigations
•Business and Personal Financial Planning
•Business Valuations
•Estate and Trust Planning
•Financial and General Business Consulting
•Tax Preparation and Planning
Services are billed at the firm's standard hourly rates plus out-of-pocket expenses.
Relburn -Metabolomics
http://relburn.com/
Man findet den Zusammenhang über Board Einträge bei Ihub der Googlen über den CEO.
"Our Mission: Relburn is a biopharmaceutical company focused on the identification, development and commercialization of metabolic drugs. Our strategy is to maximize value through excellence in performance and innovation, while maintaining the highest standards of integrity and leadership. Relburn is committed to developing innovative products to better the lives of people with chronic disorders of metabolism."
The principals of our Company have extensive experience in discovering new drugs, optimizing lead compounds, pulling these leads to IND-ready FDA submissions and into clinical development from Phase 0 through Phase 4. Generally, we expect to take our candidates through completion of randomized Phase 2 studies, such that they are “Phase 3 ready”, and then to seek partners for final development, regulatory approval, and commercialization. In unusual circumstances where Relburn can identify rapid approval pathways with limited risk, the Company may provide or secure financing for late-stage development, such that products can be partnered at a “market-ready” stage. We believe these two inflection points will maximize value for our investors.
Our current focus is on compounds that have already been tested in human subjects, but – for one reason or another – have not been optimized for use in patients with metabolic disease. Such use necessarily implies an expectation of extended, perhaps lifelong, treatment of chronic disease states. Except in highly refractory patients or acutely life-threatening exacerbations, demonstration of acceptable safety of repetitive dosing in human subjects is a paramount consideration for our involvement. Thus, prior testing of drug prototypes or analogs in human subjects provides us with a markedly higher level of confidence. We are also focused on drugs whose effectiveness has been documented within a metabolic pathway of interest. Such clinical-stage “proof-of-concept” also reduces risk going forward, identifies markets of interest and size, and clarifies regulatory pathways to approval.
Relburn is currently working on two discrete projects that have these fundamental characteristics.
" .... and then to seek partners for final development, regulatory approval, and commercialization. "
Die Firma besteht nur aus 2 Personen, Dr. Warrel: http://relburn.com/management-team/
und Dr. Piwinski: http://relburn.com/john-piwinski/
Aufgrund der Grösse und des beschriebenen Tätigkeitsfeldes kann mal also annehmen, dass die Firma nichts selbst entwickelt, sondern vermittelnd für Investoren tätig ist.
Selected Publications
F. Bennett, H. S. Kezar III, V. Girijavallabhan, Y. Huang, R. Huelgas, R. Rossman, N.-Y. Shih, J. J. Piwinski, M. MacCoss, C. D. Kwong, J. L. Clark, A. T. Fowler, F. Geng, A. Roychowdhury, R. C. Reynolds, J. A. Maddry, S. Ananthan, J. A. Secrist III, C. Li, R. Chase, S. Curry, H.-C. Huang, X. Tong, F. G. Njoroge, A. Arasappan: Pyridofuran Substituted Pyrimidine Derivatives as HCV Replication (Replicase) Inhibitors. Bioorg. Med. Chem. Lett. 22: 5144, 2012.
R. Kuang, H.-J. Shue, L. Xiao, D. Blythin, N.-Y. Shih, X. Chen, D. Gu, J. Schwerdt, L. Lin, P. C. Ting, J. Cao, R. Aslanian, J. J. Piwinski, D. Prelusky, P. Wu, J. Zhang, X. Zhang, C. S. Celly, M. Billah, P. Wang: Discovery of Oxazole-Based PDE-4 Inhibitors with Picomolar Potency. Bioorg. Med. Chem. Lett. 22: 2594, 2012.
Arasappan, F. Bennett, S. L. Bogen, S. Venkatraman, M. Blackman, K. Chen, S. Hendrata, Y. Huang, R. M. Huelgas, L. Nair, A. I. Padilla, W. Pan, R. Pike, P. Pinto, S. Ruan, M. Sannigrahi, F. Velazquez, B. Vibulbhan, W. Wu, W. Yang, A. K. Saksena, V, Girijavallabhan, N.-Y. Shih, J. Kong, T. Meng, Y. Jin, J. Wong, P. McNamara, A. Prongay, V. Madison, J. J. Piwinski, K.-C. Cheng, R. Morrison, B. Malcolm, X. Tong, R. Ralston, F. G. Njoroge, “Discovery of Narlaprevir (Sch 900518): A Potent, Second Generation HCV NS3 Serine Protease Inhibitor. ACS Med. Chem. Lett. 1: 64, 2010.
W. Yu, Z. Guo, P. Orth, V. Madison, L. Chen, C. Dai, R. J. Feltz, V. M. Girijavallabhan, S. H. Kim, J. A. Kozlowski, B. J. Lavey, D. Li, D. J. Lundell, X. Niu, J. J. Piwinski, J. Popovici-Muller, R. Rizvi, K. E. Rosner, B. B. Shankar, N. –Y. Shih, M. A. Siddiqui, J. Sun, L. Tong, S. Umland, M. K. C. Wong, D.Y. Yang, G. Zhou: Discovery and SAR of Hydantoin TACE Inhibitors. Bioorg. Med. Chem. Lett. 20: 1877, 2010.
K. E. Rosner, Z. Guo, P. Orth, G. W. Shipps, Jr., D. B. Belanger, T.-Y. Chan, P. J. Curran, C. Dai, Y. Deng, V. M. Girijavallabhan, L. Hong, B. J. Lavey, J. F. Lee, D. Li, Z. Liu, J. Popovici-Muller, P. C. Ting, H. Vaccaro, L. Wang, T. Wang, W. Yu, G. Zhou, X. Niu, J. Sun, J. A. Kozlowski, D. J. Lundell, V. Madison, B. McKittrick, J. J. Piwinski, N.-Y. Shih, M. A. Siddiqui, C. O. Strickland. The Discovery of Novel Tartrate-Based TNF-α Converting Enzyme (TACE) Inhibitors. Bioorg. Med. Chem. Lett. 20: 1189, 2010.
R. Aslanian, J. J. Piwinski, X. Zhu, T. Priestley, S. Serota, X.-Y. Du, X.-S. Zhang, R. L. McLeod, R. West, S. M. Williams, J. A. Hey: Structural Determinants for Histamine H1 Affinity, hERG Affinity and QTc Prolongation in a Series of Terfenadine Analogs. Bioorg. Med. Chem. Lett. 19: 5043, 2009.
G. Chen, I. Daaro, B. N. Pramanik, J. J. Piwinski: Structural Characterization of In Vitro Rat Liver Microsomal Metabolites of Antihistamine Desloratadine Using LTQ-Orbitrap Hybrid Mass Spectrometer in Combination with Online Hydrogen/Deuterium Exchange HR-LC/MS. J. Mass Spectrum 44: 203, 2009.
F. G. Njoroge, K. X. Chen, N.-Y. Shih, J. J. Piwinski: Challenges in Modern Drug Discovery: A Case Study of Boceprevir, an HCV Protease Inhibitor for the Treatment of Hepatitis C Virus Infection. Accts. Chem. Res. 41: 50, 2008.
S. Venkatraman, S. L. Bogen, A. Arasappan, F. Bennett, K. Chen, E. Jao, Y-T. Liu, R. Lovey, S. Hendrata, Y. Huang, W. Pan, T. Parekh, P. Pinto, V. Popov, R. Pike, S. Ruan, B. Santhanam, B. Vibulbhan, W. Wu, W. Yang, J. Kong, X. Liang, J. Wong, R. Liu, N. Butkiewicz, R. Chase, A. Hart, S. Agrawal, P. Ingravallo, J. Pichardo, R. Kong, B. Baroudy, B. Malcolm, Z. Guo, A. Prongay, V. Madison, L. Broske, X. Cui, K-C. Cheng, Y. Hsieh, J-M. Brisson, D. Prelusky, W. Korfmacher, R. White, S. Bogdanowich-Knipp, A. Pavlovsky, P. Bradley, A. K. Saksena, A. Ganguly, J. J. Piwinski, V, Girijavallabhan, F. G. Njoroge: Discovery of (1R,5S)-N-(3-Amino-1-[cyclobutylmethyl)-2,3-dioxopropyl]-3-[2(S)-[[[(1,1-dimethylethyl) amino]carbonyl]amino]-3,3-dimethyl-1-oxobutyl]-6,6-dimethyl-3-azabicyclo[3.1.0]hexan-2(S)-carboxamide (Sch 503034), a Selective, Potent, Orally Bioavailable Hepatitis C Virus NS3 Protease Inhibitor: A Potential Therapeutic Agent for the Treatment of Hepatitis C Infection. J. Med. Chem. 49: 6074, 2006.
C. L. Strickland, P. C. Weber, W. T. Windsor, Z. Wu, H. V. Le, M. M. Albanese, C. S. Alvarez, D. Cesarz, J del Rosario, J. Deskus, A. K. Mallams, F. G. Njoroge, J. J. Piwinski, S. Remiszewski, R. R. Rossman, A. G. Taveras, B. Vibulbhan, R. J. Doll, V. Girijavallabhan and A. K. Ganguly: Tricyclic Farnesyl Protein Transferase Inhibitors: Crystallographic and Colorimetric Studies of Structure-Activity Relationships. J. Med. Chem., 42, 2125, 1999.
Sollte das Gericht aber darüber entscheiden müssen, ob Assets vorhanden sind, und ob diese verwertbar sind, so muss die Prüfung erst abgewartet werden.
Die Prüfung erfolgt diese Tage, Anfang/Mitte April. Wenn verwertbare Assets verhanden sind, dann könnten Aktionäre hoffen, etwas abzubekommen, denn der Treuhänder wird versuchen, diese Assets bestmöglich zu verkaufen. Der Treuhänder verwaltet also kommisarisch die Werte der Firma, auch wenn der Besitz an der Firma bei den Aktionären liegt. Wenn Werte auftauchen/vorhanden sind, können die an das Gericht geltend gemachten Ansprüche der Direktoren (als Gläubiger) befriedigt werden.
Ich bin wie ich bin. Die einen kennen mich, die anderen können mich.
Die mit der Prüfung von Firmenbesitz beauftragte Fa. ApTo Solutions Inc. sitzt in Atlanta, und hat eine 9-jährige Expertise in der Bewertung/Abwicklung von Firmen, die sich in Chapter 7 befinden.
Dazu lese man einfach deren Seiten hier:
http://www.aptosolutions.com/services/...s/strategic-remarketing.aspx
und auch erfolgreiche Beispiele hier:
http://www.aptosolutions.com/services/...dation/view-full-resume.aspx
das nicht. Und wer diese Aktie nicht mag der schreibt hier auch nichts.
http://www.patentgenius.com/assignee/GentaInc.html
Viel interessanter sind aber die neueren Patente. Und da findet man welche hier:
http://www.faqs.org/patents/assignee/genta-incorporated/
Ein Schwerpunkt liegt darin, dass Genta versucht hat Ganite (Gallium-containing compounds) zu neuen Anwendungen zu verhelfen. Davon zeugt auch der Versuch, dass sich Ganite im IND status bei neuen Behandlungsmethoden befindet:
Quelle: http://clinicaltrials.gov/ct2/show/nct01093521