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AMUVATINIB
AMUVATINIB
| Name | N-(3,4-Methylenedioxiphenylmethyl) -4 – (benzofuro [3,2-d] pyrimidin-4-yl) piperazine-1-carbothioamide. |
| CAS | 850879-09-3 |
| Formula | C 23 H 21 N 5 O 3 S |
| MW | 447.51 |
| Synonim | MN-470, SGI-0470-03 |
Amuvatinib (MP-470) is an orally bioavailable synthetic carbothioamide with potential antineoplastic activity. Multitargeted receptor tyrosine kinase inhibitor MP470 binds to mutant forms of the stem cell factor receptor (c-Kit; SCFR), inhibiting clinically relevant mutants of this receptor tyrosine kinase that may be associated with resistance to therapy. In addition, MP470 inhibits activities of other receptor tyrosine kinases, such as c-Met, Ret oncoprotein, and mutant forms of Flt3 and PDGFR alpha, which are frequently dysregulated in variety of tumors. This agent also suppresses the induction of DNA repair protein Rad51, thereby potentiating the activities of DNA damage-inducing agents. Mutant forms of c-Kit are often associated with tumor chemoresistance.
http://www.google.co.in/patents/EP1678166A2?cl=en
Scheme 1
EXAMPLE 34 Synthesis and Analysis of Further Illustrative Compounds Compound (111-1-3), also referred to herein as HPK56/MP-470, is an illustrative compound of the present invention having the following structure:
Analogues of (111-1 -3) were designed and synthesized in order to evaluate and optimize kinase selectivity, aqueous solubility, and to improve pharmacokinetic and pharmacodynamic profiles. Illustrative synthesis approaches for generating (111-1 -3) analogues are depicted in the synthesis schemes below. Synthesis of R-i substituted benzofuranopyrimidines was undertaken. The methyl 3-guanidinobenzofuran-2-carboxylate is prepared from methyl 3-aminobenzofuran-2-carboxylate by reacting with cyanoacetamide in presence of dioxane and dry HCI gas. The obtained guanidine is cyclized in the presence of aqueous NaOH. Similar procedures were utilized for preparing 2- substituted (111-1-3) and its analogues as depicted in the Schemes 8-10 set forth below. Introduction of -NH2 at the 2 position was utilized for various sulfonic, inorganic and hydroxyacid salts. Illustrative compounds are shown in Table 4 below.Table 4
Scheme 1
Scheme 2 Scheme 3
,-NH2 /N Cl S
EXAMPLE 35 Analysis of Compound Binding and Inhibitory Activity against c-kit Mutants
The published crystal structure of c-kit kinase (pdb code:1 PKG) and its mutated structure were used to study the mode of binding of compound (111-1-3) (HPK56/MP-470), a benzofuranopyrimidine compound, its 2-substituted analogs, and quinazoline derivatives.
(Ill- 1-3)
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Information about this agent |
According to news published on 15 Apr 2008; Research data build upon previous results showing that MP-470 exhibits anti-tumor activity in breast and prostate cancer cells. The fact that MP-470 in combination with erlotinib effectively suppressed the HER pathway suggests that concurrent administration of both compounds could represent a new treatment for prostate and breast cancers.
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References |
1. Kreidberg, Jordan A.; Qin, Shan. Method using a cMET inhibitor for the treatment of polycystic kidney disease. PCT Int. Appl. (2009), 43pp. CODEN: PIXXD2 WO 2009111529 A2 20090911 CAN 151:350826 AN 2009:1107388
2. Fujiwara, Masahiro; Fujita, Masayuki. Curing agents, adhesive curable compositions, articles and coating materials therefrom, and optical materials formed by using the compositions. Jpn. Kokai Tokkyo Koho (2008), 39pp. CODEN: JKXXAF JP 2008260894 A 20081030 CAN 149:472741 AN 2008:1303932
3. Janne, Pasi A.; Engelman, Jeffrey; Cantley, Lewis C. Methods for treating cancer resistant to ErbB therapeutics. PCT Int. Appl. (2008), 96pp. CODEN: PIXXD2 WO 2008127710 A2 20081023 CAN 149:486836 AN 2008:1282443
4. Nakagawa, Kiyoshi; Kurushima, Yoshiaki; Mizuma, Masahiro. Fabric with highly-expanded layer and process for production thereof. PCT Int. Appl. (2007), 44pp. CODEN: PIXXD2 WO 2007083641 A1 20070726 CAN 147:213021 AN 2007:815020
5. Mahadevan, D.; Cooke, L.; Riley, C.; Swart, R.; Simons, B.; Della Croce, K.; Wisner, L.; Iorio, M.; Shakalya, K.; Garewal, H.; Nagle, R.; Bearss, D. A novel tyrosine kinase switch is a mechanism of imatinib resistance in gastrointestinal stromal tumors. Oncogene (2007), 26(27), 3909-3919. CODEN: ONCNES ISSN:0950-9232. CAN 147:226484 AN 2007:613908
6. Gong, QingJie; Han, DongYu; Wang, YuRong. Experimental determination of scheelite solubility in 4.0% NaCl solution in critical region. Yanshi Xuebao (2006), 22(12), 3052-3058. CODEN: YANXEU ISSN:1000-0569. CAN 147:34728 AN 2007:301330
7. Tokunaga, Koji; Mukai, Takashi; Kishigami, Akira. Two-component weak solvent-based coating compositions with no curing interference by dewing. Jpn. Kokai Tokkyo Koho (2005), 15 pp. CODEN: JKXXAF JP 2005239815 A 20050908 CAN 143:249850 AN 2005:979155
8. Lauer, S. J.; Shuster, J. J.; Mahoney, D. H., Jr.; Winick, N.; Toledano, S.; Munoz, L.; Kiefer, G.; Pullen, J. D.; Steuber, C. P.; Camitta, B. M. A comparison of early intensive methotrexate/mercaptopurine with early intensive alternating combination chemotherapy for high-risk B-precursor acute lymphoblastic leukemia: A pediatric oncology group phase III randomized trial. Leukemia (2001), 15(7), 1038-1045. CODEN: LEUKED ISSN:0887-6924. CAN 135:338846 AN 2001:586045
9. Sen, Ayusman; Hennis, April. Palladium (II) catalyzed polymerization of norbornene and acrylates. PCT Int. Appl. (2001), 22 pp. CODEN: PIXXD2 WO 2001021670 A1 20010329 CAN 134:252774 AN 2001:228935
10. Patel, Raman; Mallin, Dan; Saunders, Keith; Tiberio, Patrick; Andries, John. Polymer compositions containing polyolefins, polar polymers and block or graft copolymer compatibilizers and their preparation. PCT Int. Appl. (1999), 25 pp. CODEN: PIXXD2 WO 9950350 A1 19991007 CAN 131:272658 AN 1999:640932
11. Koehler, Burkhard; Imai, Seisaku; Doering, Joachim; Ruesseler, Wolfgang; Dorf, Ernst Ullrich. Mixtures of polyarylene sulfides, glass fibers, and polymaleimides with good mechanical properties. Ger. Offen. (1992), 4 pp. CODEN: GWXXBX DE 4105913 A1 19920827 CAN 118:82122 AN 1993:82122
12. Itoh, Michiya; Fuke, Kiyokazu; Kobayashi, Sachiko. Direct observation of intramolecular anthracene excimer in 1,3-dianthrylpropane. Journal of Chemical Physics (1980), 72(2), 1417-18. CODEN: JCPSA6 ISSN:0021-9606. CAN 92:155340 AN 1980:155340
13. Tomillero A; Moral M A Gateways to clinical trials. Methods and findings in experimental and clinical pharmacology (2009), 31(9), 597-633. Journal code: 7909595. ISSN:0379-0355. PubMed ID 20094643 AN 2010048694
14. Tomillero A; Moral M A Gateways to clinical trials. Methods and findings in experimental and clinical pharmacology (2009), 31(8), 541-57. Journal code: 7909595. ISSN:0379-0355. PubMed ID 19967103 AN 2009808578
15. Gorrand Jean-Marie; Doly Michel; Bacin Franck Macular pigment density assessed by directional fundus reflectance. Journal of the Optical Society of America. A, Optics, image science, and vision (2009), 26(8), 1847-54. Journal code: 9800943. ISSN:1084-7529. PubMed ID 19649122 AN 2009529589
16. Tomillero A; Moral M A Gateways to clinical trials. Methods and findings in experimental and clinical pharmacology (2009), 31(4), 263-98. Journal code: 7909595. ISSN:0379-0355. PubMed ID 19557204 AN 2009445725
Italy’s Newron files Parkinson’s drug with FDA
SAFINAMIDE
cas 202825-46-5 (mesylate)
N2-{4-[(3-fluorobenzyl)oxy]benzyl}-L-alaninamide
Newron Pharmaceuticals and fellow Italy-headquartered partner Zambon have filed their investigational Parkinson’s disease treatment safinamide with regulators in the USA.
The submission to the US Food and Drug Administration is for safinamide as add-on therapy in early and mid-to late stage PD patients. Newron said the filing was based on “completion of activities agreed upon during meetings” with the FDA, noting that a marketing authorisation application was submitted to the European Medicines Agency in December.
Read more at: http://www.pharmatimes.com/Article/14-05-30/Italy_s_Newron_files_Parkinson_s_drug_with_FDA.aspx#ixzz33LlGLEt7
Safinamide (EMD 1195686) is a candidate drug against Parkinson’s disease with multiple methods of action.[1] In 2007, a Phase III clinical trial was started. It was scheduled to run until 2011.[2] The compound was originally discovered at Farmitalia-Carlo Erba and developed by Newron Pharmaceuticals, which sold the rights to Merck-Serono in 2006. In October 2011 Merck-Serono announced that they would give all rights to develop the compound back to Newron.[3]
Potential additional uses might be restless legs syndrome (RLS) and epilepsy.[4] They were being tested in Phase II trials in 2008, but no results are available.
Adverse effects
Common adverse events in clinical trials were nausea, dizziness, tiredness, headache and backache. There was no significant difference in the occurrence of these effects between safinamide and placebo treated patients.[5]
Methods of action
Parkinson and RLS relevant mechanisms
Safinamide is a reversible and selective monoamine oxidase B inhibitor, reducing degradation of dopamine, and a glutamate release inhibitor.[6][5] It also seems to inhibit dopamine reuptake.[7] Additionally, safinamide blocks sodium and calcium channels.[6]
References
- Fariello, RG (2007). “Safinamide”. Neurotherapeutics 4 (1): 110–116. doi:10.1016/j.nurt.2006.11.011. PMID 17199024.
- Study of Safinamide in Early Parkinson’s Disease as Add-on to Dopamine Agonist (MOTION)
- Merck Returns Rights for Safinamide to Newron, 21 October 2011.
- Chazot, PL (2007). “Drug evaluation: Safinamide for the treatment of Parkinson’s disease, epilepsy and restless legs syndrome”. Current Opinion in Investigational Drugs 8 (7): 570–579. PMID 17659477.
- H. Spreitzer (14 April 2014). “Neue Wirkstoffe – Safinamid”. Österreichische Apothekerzeitung (in German) (8/2014): 30.
- Caccia, C; Maj, R; Calabresi, M; Maestroni, S; Faravelli, L; Curatolo, L; Salvati, P; Fariello, RG (2006). “Safinamide: From molecular targets to a new anti-Parkinson drug”. Neurology 67 (7 Suppl 2): S18–23. PMID 17030736.
- Merck Serono: Vielversprechende Daten zur kognitiven Wirkung von Safinamid bei Parkinson im Frühstadium.(German) 8 June 2007.
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1-13-2012
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PHARMACEUTICAL COMPOSITION
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10-12-2011
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Pharmaceutical composition
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10-22-2004
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Methods of treating lower urinary tract disorders using sodium channell modulators
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7-16-1999
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ALPHA-AMINOAMIDE DERIVATIVES USEFUL AS ANALGESIC AGENTS
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THANKS AND REGARD’S
DR ANTHONY MELVIN CRASTO Ph.D
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FDA Breakthrough Therapy Designation: Another For Genentech And Cancer
On May 31st, Genentech (member of the Roche Group) strategically announces that the FDA grants the Breakthrough Therapy Designation (BTD) to the company’s investigational cancer immunotherapy MPDL3280A (anti-PDL1) for the treatment of Bladder Cancer. At the 50th Annual Meeting of the American Society of Clinical Oncology (ASCO), now in progress in Chicago, Dr. Thomas Powles, M.D., clinical Professor of Genitourinary Oncology, Barts Cancer Institute at the Queen Mary University of London, is presenting on May 31st, Abstract #5011 (Results of the Phase I MPDL3280A Study).
The Phase I MPDL3280A Study, a single-arm, multi-center, open label trial, shows that MPDL3280A “shrank tumors (ORR – Overall Response Rate) in 43% (13/30) of people previously treated for metastatic Urothelial Bladder Cancer (UBC), whose tumors were characterized as PD-L1 (Programmed Death Ligand-1) positive by a test being developed by Roche.”
Per the Genentech Press Release, bladder cancer:
• Is the 9th most…
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FDA May 2014 Products Receiving Orphan Designation
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The chart below identifies FDA May 2014 Products Receiving Orphan Designation as of 05/31/14 in ascending “Orphan Drug Designation Date” order.
FDA May 2014 Products Receiving Orphan Designation
| # | Generic Name/ODD Date | Sponsor Company | Indication |
| 1 | Filanesib/ 05.06 | Array BioPharma | Multiple Myeloma |
| 2 | Autologous dendritic cells pulsed with allogeneic tumor cell lysate/ 05.06 | Amphera BV (Netherlands) | Malignant Mesothelioma |
| 3 | Ex vivo cultured human mesenchymal stromal cells / 05.08 | iCell Science AB (Sweden) | Prevention of graft rejection following solid organ transplantation |
| 4 | Adalimumab/ 05.13 | AbbVie | Uveitis |
| 5 | Diazoxide choline / 05.13 | Essentialis | Prader-Willi Syndrome |
| 6 | Vasoactive intestinal peptide (VIP)-elastin-like peptide (ELP) fusion protein / 05.13 | PhaseBio Pharmaceuticals | Pulmonary arterial hypertension |
| 7 | (Z)-3-(3-(3,5-bis(trifluoromethyl)phenyl)-1H-1,2,4-triazol-1-yl)-N-(pyrazin-2-yl)acrylohydrazide / 05.14 | Karyopharm Therapeutics | Diffuse large B-cell lymphoma |
| 8 | 177Lu-tetraxetan-tetulomab / 05.14 | Nordic Nanovector AS (Norway) | Follicular Lymphoma |
| 9 | Selinexor; (Z)-3-(3-(3,5-bis(trifluoromethyl)phenyl)-1H-1,2,4-triazol-1-yl)-N-(pyrazin-2-yl)acrylohydrazide / 05.14 | Karyopharm Therapeutics | Acute myeloid leukemia |
| 10 | Menadione Sodium Bisulfite/ 05.14 |
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Cocrystals
Active pharmaceutical ingredients (APIs) are frequently delivered to the patient in the solid state as part of such dosage forms as tablets, capsules, etc.In this context the ability to deliver the drug to the patient in a safe, efficacious and cost-effective way depends largely on the physicochemical properties of the APIs in the solid state, and ……..read more
API SCALEUP (R AND D)
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| The ultimate goal of drug synthesis is to scale up from producing milligram quantities in a laboratory to producing kilogram to ton quantities in a plant, all while maintaining
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Polymer Nanoflower Encapsulates Two Cancer Drugs to Hit Tumors with More Punch
Many existing anti-cancer drugs can be disappointingly ineffective in clinical practice, but often it is the delivery method and not the medication itself that limits effectiveness. Being able to deliver multiple drugs together, each with a different mechanism of action, to their target can be considerably more powerful than separate administrations. Researchers at North Carolina State University and the University of North Carolina at Chapel Hill have developed a “nanoflower” made out of a hydrophilic polymer that carries camptothecin and doxorubicin directly into cancer cells.
The hydrophobic drugs are encapsulated within the polyethylene glycol structure similarly to how proteins fold in on themselves. At about 50 nanometers in diameter, the nanoflowers can be injected into the bloodstream to seek out cancer cells. In an animal study, the structures stayed together until they penetrated lung cancer cells by taking advantage of “lipid raft and clathrin-mediated endocytotic pathway without premature leakage,” according…
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BioCryst Pharmaceuticals Inc. ( BCRX ) will be reporting results from OPuS-1, a phase IIa trial of orally-administered BCX4161 in patients with hereditary angioedema
(RTTNews.com) – BioCryst Pharmaceuticals Inc. ( BCRX ) will be reporting results from OPuS-1, a phase IIa trial of orally-administered BCX4161 in patients with hereditary angioedema, on Tuesday, May 27, 2014 at 8:30 a.m. Eastern Time.
The OPuS-1 clinical trial is testing 400 mg of BCX4161 administered three times daily for 28 days in up to 25 hereditary angioedema patients who have a high frequency of attacks (≥ 1 per week), in a randomized, placebo-controlled, two-period cross-over design.
Read more: http://www.nasdaq.com/article/bcrx-to-watch-out-for-gtiv-adopts-poison-pill-teva-qgen-drtx-get-fda-nod-20140527-00005#ixzz335Khl0sk
BCX-4161 is a novel, selective inhibitor of plasma kallikrein in development for prevention of attacks in patients with hereditary angioedema (HAE). By inhibiting plasma kallikrein, BCX-4161 suppresses bradykinin production. Bradykinin is the mediator of acute swelling attacks in HAE patients.
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old article
BCRX – BioCryst – Entering The HAE Market
BioCryst announced on Monday July 22 the successful completion of a Phase I study on the safety and PK of BCX4161, a candidate for the treatment of Hereditary angioedema (HAE). HAE is a genetic disorder resulting from the loss or dysfunction of complement C1 Inhibitor (C1INH).
Among the functions performed by C1INH is regulation of the hormone bradykinin, which when activated, leads to the dilation of blood vessels. Left unchecked, excess bradykinin can cause painful attacks of swelling, or angioedemas, in any part of the body, including the face, abdomen, hands, and larynx. Death can occur from asphyxiation, particularly in children.
The mechanics involved in HAE are fairly well understood today. There are several approved drugs available today that work at three major points in the pathway. Ultimately, each prevents bradykinin from activating its receptor on endothelial cells.
C1 Inhibitors, of which four have been approved, prevent Factor XIIa activation of Plasma Kallikrein and inhibit Kallikrein itself. The single specific Kallikrein inhibitor is Kalbitor from Dyax. C1INHs and kallikrein inhibitors prevent the formation of bradykinin (labeled “BK” in this diagram). Then there is Firazyr from Shire, a B2 bradykinin receptor antagonist; while not preventing overproduction of the hormone, activation of downstream activity is suppressed.
Interestingly, of all the available therapies, only C1INH Cinryze from Viropharma is approved for prophylactic use- all others are designated strictly for treatment of acute attacks. A key reason for this is Cinryze’s long half-life, allowing sustained activity over longer intervals. As each of these drugs are given by injection, frequent treatment is not practical. Consider, for instance, Kalbitor has a half life of just two hours.
This is where BioCryst comes in. The company is pursuing the less crowded prophylaxis indication. It has the only orally available (although just barely) plasma kallikrein inhibitor. And while PK is not great, requiring three-times daily dosing to ensure adequate drug levels, pills make this a feasible option. As you can see, 800 mg appears optimal, however, 400 mg was selected as the Phase IIa dose due to 3 cases of moderate AEs seen at 800. This study was in healthy volunteers and the drug was otherwise well tolerated [ref].
(From Company Presentation)
BCX4161 is an interesting compound. Based on patent literature, we believe the molecule has a similar structure to the one illustrated below:
BCX4161 is not a specific inhibitor of kallikrein, and in fact has near equal potency against Factor XIIa. This dual-activity is also seen with C1INH, setting the compound apart from Kalbitor and Firazyr.
The different profile may improve efficacy, but that is unknown at this point. Along with Factor XIIa, BCX4161 inhibits additional factors involved in coagulation. Bleeding issues has been something the company has been testing and will be certain to monitor. As a drug designed for chronic use, safety will be a major concern.
A 25 patient Phase IIa study set for Q4 will be placebo-controlled double-blind crossover of the following design:
(From Company Presentation)
Individuals with a high frequency of attacks(~1/week) will be enrolled, the primary endpoint is attack frequency. Viropharma conducted a pivotal trial of similar design (but two twelve week dosing periods), reporting ~50% reduction in attacks vs. placebo. We imagine BioCryst would need to achieve results in this range for the drug to be competitive.
A major impedance toward these efficacy goals will likely be individual adherence to dosing every eight hours schedule. Missed doses will mean severe drops in drug levels, potentially putting the patient at risk for an attack. The company noted patients on Cinryze occasionally miss doses with no apparent adverse effect. We will see if this holds true for their own compound.
The Phase IIa is being run in Germany, ostensibly because of the country’s well organized HAE medical treatment system. The study is expected to initiate in 4Q 2013. BioCryst aims to market the drug in the U.S. on their own, likely partnering in the EU.
Handicapping this Phase II is rather difficult with the lack of any prior efficacy results. BioCryst has selected a well-validated target in a fairly well understood disease. The data suggests BCX4161 is an active drug. What we will soon find out is whether the compound is active enough and has a sufficiently clean profile. As attractive as oral dosing is- it has an achilles heel. Regardless of the medication, patients continue to have attacks, only of less frequency and severity. If a patient should suffer major laryngeal swelling, pills may not be an option as a rescue medicine. Cinryze on the hand can serve as both prophylaxis and acute treatment.
Commercially, we believe the compound will have a difficult time competing with Cinryze. True, Cinryze has its own issues, namely a requirement for infusions every 3 to 4 days, but it is difficult to see how a 3-times/day treatment is much of an improvement. In any case, by the time BCX4161 reaches the market, Viropharma should have a much simpler subcutaneous version of its C1INH available, allowing it to maintain a strong monopoly in prophylaxis HAE treatments. Additional competition may come in the form of a follow-up kallikrein inhibitor in development at Dyax; the long acting antibody is designed specifically for the prophylaxis market and is expected to enter the clinic 2H 2013.
आयुर्वेद न्यूट्रास्यूटीकल्स ; अधिक गर्मी के कारण होने वाली तकलीफो से बचने के लिये ………
आयुर्वेद की विशेषता यही है कि सभी मौसम के लिये सभी के लिये आयुर्वेद के मनीषियों ने मौसम से प्राप्त सभी वस्तुओ के सटीक उपयोग के लिये combinations दे दिये है /
गर्मी के मौसम मे गर्म हवाओ के चलने और लू लपट high degree temperature के चलते हुये बहुत सी तकलीफे शरीर मे अचानक पैदा होने की स्तिथि बन जाती है , इन सभी अवस्थाओ से बचने के लिये नीचे लिखे nueutraceutical को अपनाइये और फायदा उठाइये ;
साम्ग्री सब आप्के किचन मे मिल जायेगी /
१- एक छोटा प्याज , बड़ा हो तो आधा कर ले
२- एक कच्चा छोटा आम / अमिया
३-१५ -२० पुदीना की पत्ती / अधिक भी छोड़ सकते है
४- एक टुकड़ा अदरख
५- एक चम्मच जल जीरा मसाला पाउडर
५- आधा चम्मच काली मिर्च
६- स्वादानुसार काला नमक
७- एक या दो चम्मच शक्कर / चीनी / गुड़
८- आधा या…
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DR ANTHONY MELVIN CRASTO
ORGANIC SPECTROSCOPY
New Drug Approvals 