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Interferon For Treatment of Melanoma

35,643 bytes added, 07:07, 7 September 2018
==Dashboard==
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==Interactive Taxonomy==
<mm>[[Interferon_For_the_treatment_Of_Melanoma.mm|1000px]]</mm>
==Concept Table==
{|border="2" cellspacing="0" cellpadding="4" width="50100%"
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''S.No'''</center>
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''Concept-1'''</center>
|}
===French Keywords Concept table===
{|border="2" cellspacing="0" cellpadding="4" width="50100%"
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''S.No'''</center>
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''Concept-1'''</center>
===German Keywords Concept Table===
{|border="2" cellspacing="0" cellpadding="4" width="50100%"
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''S.No'''</center>
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''Concept-1'''</center>
|}
==Taxonomy==
 
[[Image:taxonomy melanoma mod1.jpg|700px|center|thumb| '''Taxonomy''']]
===Class codes identified for searches===
* '''Relevant IPC classes'''
{|border="2" cellspacing="0" cellpadding="4" width="75100%"
|align = "center" bgcolor = "#99CCFF" colspan = "4"|'''IPC'''
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''Sr. No.'''|align = "center" bgcolor = "#C0C0C099ccff"|'''Class Code'''|align = "center" bgcolor = "#C0C0C099ccff"|'''Class definition'''|align = "center" bgcolor = "#C0C0C099ccff"|'''Class coverage'''
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''1'''
|align = "center"|A61K003819
|align = "center"|Medicinal preparations containing peptides - Cytokines; Lymphokines; Interferons
|align = "center"|Broad
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''2'''
|align = "center"|A61K003821
|align = "center"|Medicinal preparations containing peptides Interferon
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''3'''
|align = "center"|C07K001452
|align = "center"|Peptides having more than 20 amino acids; Gastrins; Somatostatins; Melanotropins; Derivatives thereof - Cytokines; Lymphokines; Interferons
|align = "center"|Broad
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''4'''
|align = "center"|C07K014555
|align = "center"|Peptides having more than 20 amino acids - Interferon
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''5'''
|align = "center"|C07K001456
|align = "center"|Peptides having more than 20 amino acids - IFN-alpha
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''6'''
|align = "center"|C07K014565
|align = "center"|Peptides having more than 20 amino acids - IFN-beta
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''7'''
|align = "center"|C07K001457
|align = "center"|Peptides having more than 20 amino acids - IFN-gamma
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''8'''
|align = "center"|A61P003500
|align = "center"|Therapeutic activity of chemical compounds or medicinal preparations -antineoplastic agents
* '''Relevant ECLA classes'''
{|border="2" cellspacing="0" cellpadding="4" width="75100%"
|align = "center" bgcolor = "#99CCFF" colspan = "4"|'''ECLA'''
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''Sr. No.'''|align = "center" bgcolor = "#C0C0C099ccff"|'''Class Code'''|align = "center" bgcolor = "#C0C0C099ccff"|'''Class definition'''|align = "center" bgcolor = "#C0C0C099ccff"|'''Class coverage'''
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''1'''
|align = "center"|A61K003819
|align = "center"|Medicinal preparations containing peptides - Cytokines; Lymphokines; Interferons
|align = "center"|Broad
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''2'''
|align = "center"|A61K003821
|align = "center"|Medicinal preparations containing Interferon
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''3'''
|align = "center"|A61K38/21A
|align = "center"|Medicinal preparations containing IFN-alpha
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''4'''
|align = "center"|A61K38/21B
|align = "center"|Medicinal preparations containing IFN-beta
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''5'''
|align = "center"|A61K38/21C
|align = "center"|Medicinal preparations containing IFN-gamma
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''6'''
|align = "center"|C07K001452
|align = "center"|Peptides having more than 20 amino acids; Gastrins; Somatostatins; Melanotropins; Derivatives thereof - Cytokines; Lymphokines; Interferons
|align = "center"|Broad
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''7'''
|align = "center"|C07K014555
|align = "center"|Peptides having more than 20 amino acids - Interferon
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''8'''
|align = "center"|C07K001456
|align = "center"|Peptides having more than 20 amino acids - IFN-alpha
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''9'''
|align = "center"|C07K014565
|align = "center"|Peptides having more than 20 amino acids - IFN-beta
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''10'''
|align = "center"|C07K001457
|align = "center"|Peptides having more than 20 amino acids - IFN-gamma
|align = "center"|Specific
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''11'''
|align = "center"|C07K014715G
|align = "center"|Receptors; Cell surface antigens; Cell surface determinants - for interferons -
* '''Relevant US classes'''
{|border="2" cellspacing="0" cellpadding="4" width="50100%"
|align = "center" bgcolor = "#99CCFF" colspan = "3"|'''US class'''
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''Sr. No.'''|align = "center" bgcolor = "#C0C0C099ccff"|'''Class Code'''|align = "center" bgcolor = "#C0C0C099ccff"|'''Class definition'''
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''1'''
|align = "center"|4240854
|align = "center"|DRUG, BIO-AFFECTING AND BODY TREATING COMPOSITIONS - this subclass provides for patents which broadly claim interferon or a method of treatment of interferon where the classification of the interferon as alpha, beta or gamma interferon is impossible
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''2'''
|align = "center"|4242811
|align = "center"| DRUG, BIO-AFFCTING AND BODY TREATING COMPOSITIONS - Virus (e.g., interferon-inducing virus, etc.)
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''3'''
|align = "center"|42400141
|align = "center"|DRUG, BIO-AFFECTING AND BODY TREATING COMPOSITIONS - Attached to lymphokine, cytokine, or other secreted growth regulatory factor, differentiation factor, or intercellular mediator specific for a hematopoietic cell (e.g., interferon, interleukin, macrophage factor, colony stimulating factor, erythropoietin); derivative thereof
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''4'''
|align = "center"|514889
|align = "center"|DRUG, BIO-AFFECTING AND BODY TREATING COMPOSITIONS - INTERFERON INDUCER
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''5'''
|align = "center"|530351
|align = "center"| CHEMISTRY: NATURAL RESINS OR DERIVATIVES; PEPTIDES OR PROTEINS; LIGNINS OR REACTION PRODUCTS THEREOF - Lymphokines, e.g., interferons, interlukins, etc.
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''6'''
|align = "center"|930142
|align = "center"|PEPTIDE OR PROTEIN SEQUENCE - Interferon
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''7'''
|align = "center"|4240851
|align = "center"|LYMPHOKINE - Included in this and the indented subclasses interferon, interleukin and macrophage factors (monokines)
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''8'''
|align = "center"|4240855
|align = "center"|Gamma or immune: This subclass is indented under subclass 85.4. Subject matter in which the interferon is gamma or immune interferon.
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''9'''
|align = "center"|4240856
|align = "center"|Subject matter in which the interferon is beta or fibroblast interferon.
|-
|align = "center" bgcolor = "#C0C0C099ccff"|'''10'''
|align = "center"|4240857
|align = "center"|Subject matter in which the interferon is alpha or leukocyte interferon.
===Search strategy and concept===
Date of Search: 1836 to October 26Feb 3rd, 2009 2011
Database used: Micropatent - Include extensive full text and MPI-Inpadoc searches
{|border="2" cellspacing="0" cellpadding="4" width="100%"
|align = "center" bgcolor = "#99CCFF"|'''SrS. No.'''
|align = "center" bgcolor = "#99CCFF"|'''Search concept'''
|align = "center" bgcolor = "#99CCFF"|'''Search Scope'''
|align = "center" bgcolor = "#99CCFF"|'''No. of hits'''
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''1'''
|align = "center"|Interferon for treating Melanoma
|align = "center"|Title, Abstract and Claims
|align = "center"|576
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''2'''
|align = "center"|Interferon for treating Melanoma
|align = "center"|Title, Abstract and Claims
|align = "center"|756
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''3'''
|align = "center"|'''Final query'''
|align = "center" colspan = "4"|'''1 OR 2'''
{|border="2" cellspacing="0" cellpadding="4" align = "center" width="100%"
|align = "center" bgcolor = "#99CCFF"|'''SrS. No.'''
|align = "center" bgcolor = "#99CCFF"|'''Search concept'''
|align = "center" bgcolor = "#99CCFF"|'''Language'''
|-
|}
 
===Search in Micropatent MPI-INPADOC - English language search===
{|border="2" cellspacing="0" cellpadding="4" width="100%"
|align = "center" bgcolor = "#99CCFF"|'''SrS. No.'''
|align = "center" bgcolor = "#99CCFF"|'''Search concept'''
|align = "center" bgcolor = "#99CCFF"|'''Search Scope'''
|align = "center" bgcolor = "#99CCFF"|'''No. of hits'''
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''1'''
|align = "center"|Interferon for treating Melanoma
|align = "center"|Title and Abstract
|align = "center"|174
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''2'''
|align = "center"|Interferon for treating Melanoma
|align = "center"|Title and Abstract
|align = "center"|484
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''3'''
|align = "center"|Interferon for treating Melanoma
|align = "center"|Title and Abstract
|align = "center"|102
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''4'''
|align = "center"|Interferon for treating Melanoma
|align = "center"|Title and Abstract
|align = "center"|9
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''5'''
|align = "center" colspan = "4"|'''Final query'''
|align = "center"|'''1 OR 2 OR 3 OR 4'''
{|border="2" cellspacing="0" cellpadding="4" width="100%"
|align = "center" bgcolor = "#99CCFF"|'''SrS. No.'''
|align = "center" bgcolor = "#99CCFF"|'''Search concept'''
|align = "center" bgcolor = "#99CCFF"|'''Language'''
Database: IPDL (Industrial property digital library), Japan
Date of search: 1900/01/01 to 20092011/1002/2615 {| border="2" cellspacing="0" cellpadding="4" align = "left" width="100%"| style="background-color:#99ccff;padding:0.079cm;"| '''S.No.'''| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Issue/Publication date'''</center>| style="background-color:#99ccff;padding:0.079cm;"| <center>'''F-Term Theme'''</center>| style="background-color:#99ccff;padding:0.079cm;"| <center>'''FI/F-term/Facet '''</center>| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Hits'''</center> |-| style="background-color:#99ccff;padding:0.079cm;"| <center>'''1'''</center>| style="padding:0.079cm;"| <center>'''1900/01/01 to 2011/02/15'''</center>| style="padding:0.079cm;"| <center>4H045</center>| style="padding:0.079cm;"| <center>DA15+DA16+DA17+DA18 </center>| style="padding:0.079cm;"| <center>1298</center> |} <br>  '''Total patents: 1298 (Relevancy ~10%)'''
'''Total patents: 846 (Relevancy ~10%)'''
* '''F-Terms and theme used in search'''
{|border="2" cellspacing="0" cellpadding="4" width="75100%"
|align = "center" bgcolor = "#99CCFF" colspan = "3"|'''Japanese F-term search'''
|align = "center" bgcolor = "#99CCFF"|'''Definition'''
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''Sr. No.'''
|align = "center"|'''F- Term theme'''
|align = "center"|'''4H045'''
|align = "center"|Peptides having more than 20 amino acids; Gastrins; Somatostatins; Melanotropins; Derivatives thereof
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''1'''
|align = "center"|F-term
|align = "center"|DA15
|align = "center"|Peptide or protein characterised by function - Interferons
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''2'''
|align = "center"|F-term
|align = "center"|DA16
|align = "center"|Alpha-interferons
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''3'''
|align = "center"|F-term
|align = "center"|DA17
|align = "center"|Beta-interferons
|-
|align = "center" bgcolor = "#C0C0C099CCFF"|'''4'''
|align = "center"|F-term
|align = "center"|DA18
|align = "center"|Gamma-interferons
|-
|}
 
===Scientific Literature Search===
 
{|border="2" cellspacing="0" cellpadding="4" width="100%"
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>S.No</b></center>
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>Database</b></center>
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>Query</b></center>
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>Limits by Date</b></center>
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>No.Of Hits</b></center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>1</b></center>
| style="padding:0.079cm;"| <center>Pubmed</center>
| style="padding:0.079cm;"| <center>(Melanoma Or carcinoma or cancer* or tumor) And (IFN* OR Interferon)</center>
| style="padding:0.079cm;"| <center>20000101-20110221</center>
| style="padding:0.079cm;"| <center>28402</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>2</b></center>
| style="padding:0.079cm;"| <center>Scirus</center>
| style="padding:0.079cm;"| <center>(Melanoma Or carcinoma or cancer* or tumor) And (IFN* OR Interferon)</center>
| style="padding:0.079cm;"| <center>2000-2011</center>
| style="padding:0.079cm;"| <center>24835</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>3</b></center>
| style="padding:0.079cm;"| <center>Google Scholar</center>
| style="padding:0.079cm;"| <center>(Melanoma Or carcinoma or cancer* or tumor) And (IFN* OR Interferon)</center>
| style="padding:0.079cm;"| <center>2000-2011</center>
| style="padding:0.079cm;"| <center>21100</center>
 
|}
{|border="2" cellspacing="0" cellpadding="4" width="100%"
|align = "center" bgcolor style= "background-color:#C0C0C099ccff;;padding:0.079cm;"|<center>'''S.No.'''</center>|align = "center" bgcolor style= "background-color:#99CCFF99ccff;;padding:0.079cm;"|<center>'''Patent/Publication No.'''</center>|align = "center" bgcolor style= "background-color:#99CCFF99ccff;;padding:0.079cm;"|<center>'''Date of Of Publication'''</center>|align = "center" bgcolor style= "background-color:#99CCFF99ccff;;padding:0.079cm;"|<center>'''Assignee / Applicant'''</center>|align style= "centerbackground-color:#99ccff;;padding:0.079cm;" bgcolor | <center>'''Title'''</center>| style= "background-color:#99CCFF99ccff;;padding:0.079cm;"|<center>'''Inventor(s)Abstract'''</center>|align = "center" bgcolor style= "background-color:#99CCFF99ccff;;padding:0.079cm;"|<center>'''TitleProblem'''</center>|align = "center" bgcolor style= "background-color:#C0C0C099ccff;;padding:0.079cm;"|<center>'''Dolcera SummarySolution'''</center> 
|-
|align = "center" bgcolor style= "background-color:#C0C0C099ccff;;padding:0.079cm;"|<center>'''1'''</center>|align style= "center;padding:0.079cm;"|<font color="#0000FF"><ucenter>[http://v3patft.espacenetuspto.comgov/publicationDetailsnetacgi/biblionph-Parser?DBSect1=EPODOCPTO1&adjacentSect2=trueHITOFF&localed=en_EPPALL&FTp=D1&dateu=20051027%2Fnetahtml%2FPTO%2Fsrchnum.htm&CCr=US1&NRf=2005238621A1G&KCl=A1 50&s1=7482014.PN.&OS=PN/7482014&RS=PN/7482014 US7482014B2]</u></fontcenter>|align style= "center;padding:0.079cm;"|1<center>01/27/2009</center>|align style= "center;padding:0.079cm;"|<center>Schering Corporation</center>|align style= ";padding:0.079cm;"| <center>Melanoma therapy </center>| style=";padding:0.079cm;"|Rybak<center>Methods for treating treatment-naive as well as treatment-experienced patients having melanoma to increase the progression-free survival time involving administering a therapeutically effective amount of pegylated interferon-alpha, Mary Ellen and Rosee.g., Esther Helenpreferably pegylated interferon alpha-2b, as adjuvant therapy to definitive surgery are disclosed.</center>|align style= "center;padding:0.079cm;"|<center>The problem is with the treatment methods that are employed with previously employed dose regimens for treating Melanoma therapyafter definitive surgical removal of the lesions.This led to the occurance of hematologic, neurologic and constitutional toxicities.Subject compliance with the dosage and dosage regimen during both phases is considered to be important to achieve maximum clinical benefit. </center>|align style= "center;padding:0.079cm;"|<center>The invention relates to a method higher patience compliance is achieved with the improved methods of treatment of treating a patient having Stage IIB or Stage III melanoma which has been surgically removed. A therapeutically effective dose of pegylated interferon alpha for a time period sufficient to increase the progression-free survival time was administered to the patient.The treatment regimen includes a first dose of 6.0 micrograms/kg of pegylated PEG.sub.12000 interferon alpha-2b once a week for eight weeks, and then administering to the patient a second dose of 3.0 or less micrograms/kg of pegylated PEG.sub.12000 interferon alpha-2b once a week for the remainder of a five year treatment period.</center> 
|-
|align = "center" bgcolor style= "background-color:#C0C0C099ccff;;padding:0.079cm;"|<center>'''2'''</center>|align style= "center;padding:0.079cm;"|<font color="#0000FF"><ucenter>[http://v3patft.espacenetuspto.comgov/publicationDetailsnetacgi/biblionph-Parser?DBSect1=EPODOCPTO1&adjacentSect2=trueHITOFF&localed=en_EPPALL&FTp=D1&dateu=19991207%2Fnetahtml%2FPTO%2Fsrchnum.htm&CCr=US1&NRf=5997858AG&KCl=A 50&s1=5997858.PN.&OS=PN/5997858&RS=PN/5997858 US5997858A]</u></fontcenter>|align style= "center;padding:0.079cm;"|<center>12/7/1999</center>|align style= "center;padding:0.079cm;"|<center>Pharma Pacific Pty Ltd.|align = "</center"|Tovey, Michael Gerard and Kaido, Thomas James>|align style= "center;padding:0.079cm;"|<center>Stimulation of host defense mechanisms against tumors</center>|align style= "center;padding:0.079cm;"|<center>A method for treating multiple myeloma, hairy cell leukemia, malignant melanoma, brain tumors etc. by neoplastic disease in a mammal via administering to the mammal a therapeutically effective amount of an interferon (via oromucosal contact. The amount of interferon administered is less than an amount which induces a pathological response when administered parenterally.</center>| style=";padding:0.079cm;"| <center>The problem is with the method employed for the treatment of neoplastic diseases.The administration of low doses of interferon as a nasal spray or as an oral liquid formulation in the treatment of the neoplastic diseases is not effective in the previous patents.There is no experimental evidence regarding the administration mode of the interferon,though it was anticipated that administrations through other modes is possible to deliver effectively and treating the same conditions.</center>| style=";padding:0.079cm;"| <center>The solution to the problem is solved by first controlled study in an animal model of the efficacy of oromucosally administered interferon for the treatment of neoplastic diseases.The administration is done oromucosally in asingle dose by almost all forms of Interferons .the amount administered is from about 1500 IU to about 20×10<20.times.10.sup>.6</sup> IU for a 70 kg man per day) via oromucosal contact.This amount is less than the amount that induces a pathological response in the mammal when administered parenterally.</center> 
|-
|align = "center" bgcolor style= "background-color:#C0C0C099ccff;;padding:0.079cm;"|<center>'''3'''</center>|align style= "center;padding:0.079cm;"|<font color="#0000FF"><ucenter>[http://v3.espacenet.com/publicationDetails/biblio?DB=EPODOC&adjacent=true&locale=en_EP&FT=D&date=19881026&CC=EP&NR=0288055A1&KC=A1 EP288055A1]</u></fontcenter>|align style= "center;padding:0.079cm;"|<center>10/26/1988</center>|align style= "center;padding:0.079cm;"|<center>MERRELL DOW PHARMACEUTICALS INC.</center>|align style= "center;padding:0.079cm;"|Sunkara, Sai P.|align = "<center"|>Use of ODC inhibitors, dacarbazine, and interferon, in the treatment of malignant melanoma</center>|align style= "center;padding:0.079cm;"|A combinational <center>This invention relates to the improvement of the polyamine depletion effects of ornithine decarboxylase inhibitors, the improvement being effected by the use of Interferon and Dacarbazine in conjunctive therapy with said inhibitors.</center>| style=";padding:0.079cm;"| <center>The problem in this patent is associated with the methods and drugs that are used for treating the pathological disease conditions such as cancer.Polyamines mechanism is not known and there are some evidences that ODC inhibitors may exert their therapeutic effect by blocking the formation of the polyamines and thereby slowing, interrupting, or arresting the proliferation and metastases of the tumor tissue. So certain methods are explored to find out the same kind of effect on treating cancers.</center>| style=";padding:0.079cm;"| <center>The solution was found to be the improved methods in treating the cancer with the use of Interferon and Dacarbazine when these disease states are treated with irreversible inhibitors of ornithine decarboxylase.This includes a pharmaceutical product containing an ornithine decarboxylase inhibitor, Interferon and Dacarbazine as a combined preparation for simultaneous, separate or sequential use in treating rapidly-proliferating cell-growth disease such as melanomastates.Even the methods for the formulation are disussed in this patent.</center> 
|-
|align = "center" bgcolor style= "background-color:#C0C0C099ccff;;padding:0.079cm;"|<center>'''4'''</center>|align style= "center;padding:0.079cm;"|<font color="#0000FF"><ucenter>[http://v3.espacenet.com/publicationDetails/biblio?DB=EPODOC&adjacent=true&locale=en_EP&FT=D&date=19871014&CC=EP&NR=0241242A1&KC=A1 EP241242A1]</u></fontcenter>|align style= "center;padding:0.079cm;"|<center>10/14/1987</center>|align style= "center;padding:0.079cm;"|<center>CETUS ONCOLOGY CORPORATION|align = "</center"|Rudolph, Alfred>|align style= "center;padding:0.079cm;"|<center>The use of interferon-beta and interleukin-2 for combination therapy and compositions therefor</center>|align style= "center;padding:0.079cm;"|A <center>Anti-tumor activity in humans can be augmented by administering to the human patient and effective amount of IFN-&#946; and IL-2 in combination. The composition comprising of IFN-&#946; and IL-2 may be prepared invitro or administered separately to the patient. The composition is useful for prophylactic or therapeutic treatment of such cancers as melanoma, colon cancer lung cancer and breast cancer.</center>| style=";padding:0.079cm;"| <center>The problem in this patent is about the use of interferons seperately in treating the cancers.When administered seperately they were found to induce a mixture response that was good.So an approach was thought of lFN- where the combination therapy was given to produce better results.</center>| style=";padding:0.079cm;"| <center>The concern of the prior art was addressed with the successful administration of a combination therapy with Interferon beta and ILinterleukin-2 as an anti-tumor therapeutic or prophylactic agent. It was made suitable for administration to human patients for therapeutic or prophylactic treatment of cancer such as colon cancercomprising formulating together, melanoma, renal cell cancer, lung cancerwhether by mixing or providing separate doses.The administration is done parenterally.</center> 
|-
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''5'''</center>
| style=";padding:0.079cm;"| <center>[http://appft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PG01&p=1&u=%2Fnetahtml%2FPTO%2Fsrchnum.html&r=1&f=G&l=50&s1=%2220100086518%22.PGNR.&OS=DN/20100086518&RS=DN/20100086518 US20100086518] </center>
| style=";padding:0.079cm;"| <center>4/8/2010</center>
| style=";padding:0.079cm;"| <center>NOVARTIS AG</center>
| style=";padding:0.079cm;"| <center>Treatment of melanoma</center>
| style=";padding:0.079cm;"| <center>Methods of treating melanoma include administering a compound of Structure I, a tautomer of the compound, a pharmaceutically acceptable salt of the compound, a pharmaceutically acceptable salt or the tautomer, or a mixture thereof to a subject. The compound, tautomer, salt of the compound, salt of the tautomer, or mixture thereof may be used to prepare medicaments for treating metastatic cancer. The variable A has the values defined herein.</center>
| style=";padding:0.079cm;"| <center>The problem is that though there are many methods of treating cancer , still there is a need for the advancements in the technologies to be adopted to arrive at better results.The compounds such as quinoline derivatives were used and were disclosed in the prior art for the treatment of Melanoma.The compounds that were used previously were found to be associated with the side effects.</center>
| style=";padding:0.079cm;"| <center><nowiki>The solution was found to be finding of compounds that can effectively administered for treating Melanoma.It relates to the use of compounds such as 4-amino-5-fluoro-3-[6-(4-methylpiperazin-1-yl)-1H-benzimidazol-2-yl]quino- lin-2(1H)-one and tautomers, salts, and mixtures thereof in treating melanoma and preparing medicaments for treating melanoma. The therapeutically effective amount of the compound can range from about 0.25 mg/kg to about 30 mg/kg body weight of the subject.</nowiki></center>
 
|-
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''6'''</center>
| style=";padding:0.079cm;"| <center>[http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=4846782.PN.&OS=PN/4846782&RS=PN/4846782 US4846782] </center>
| style=";padding:0.079cm;"| <center>7/11/1989</center>
| style=";padding:0.079cm;"| <center>Schering Corporation</center>
| style=";padding:0.079cm;"| <center>Treatment of cancer with interferon and radiotherapy </center>
| style=";padding:0.079cm;"| <center>Radiation sensitive human cancers are treated with combined interferon and radiation therapy.</center>
| style=";padding:0.079cm;"| <center>Radiation therapy emerged some years back for the treatment of cancers.It was observed that the results are good.But there was a need felt to effectively increase the efficacy of radiation treatment.So to develop radiation sensitizers or potentiators which enable the radiation to cause increased tumor destruction. Despite numerous laboratory and clinical studies, no single agent has, to date, emerged as the optimal radiation sensitizer. </center>
| style=";padding:0.079cm;"| <center>The problem could be addressed by an effective treatment means using administering subcutaneously to such patients between 2.0.times.10.sup.6 IU/m.sup.2 and 5.0.times.10.sup.6 IU/m.sup.2 of recombinant DNA-alpha-2-interferon .This is done three days a week at a time on those days prior to radiation therapy.The doses are from 15 to 35 Gy are administered five days a week including those days on which interferon is administered.</center>
 
|-
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''7'''</center>
| style=";padding:0.079cm;"| <center>[http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=5824300.PN.&OS=PN/5824300&RS=PN/5824300 US5824300] </center>
| style=";padding:0.079cm;"| <center>10/20/1998</center>
| style=";padding:0.079cm;"| <center>The Texas A&M University System</center>
| style=";padding:0.079cm;"| <center>Treatment of neoplastic disease with oral interferon </center>
| style=";padding:0.079cm;"| <center>Neoplastic diseases are treated by the administration of human interferon, particularly IFN-&#945;, at a dosage of from about 0.01 to about 5 IU/lb./day such that the interferon is held in contact with the patient's oral and pharyngeal mucosae. The interferon is administered in a solid dosage from, e.g., a saliva-dissolvable lozenge.</center>
| style=";padding:0.079cm;"| <center>Though the research is intensive in the field of interferons,there exists a substantial lack of uniformity in such matters as classification of interferon types. There are also numerous, sometimes contradictory, theories concerning the mode of action of interferon in producing clinical effects.It became apparent that exogenous interferon was sometimes capable of effecting regression or remission of various metastatic diseases. so different studies are conducted to know the clinical agent of choice for the prevention of cancers.</center>
| style=";padding:0.079cm;"| <center>The present invention is based on applicant's discovery that interferon can be used as a consistently effective therapeutic agent for treatment of diseases having an immunopathologic basis--characterized by inadequate immune response and persistence of the disease.The interferon is administered in an amount of about 0.01 to about 5 IU/lb of patient body weight per day. Multiple dose daily regimen is given to the patients.They aid in the better treatment of cancers.</center>
 
|-
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''8'''</center>
| style=";padding:0.079cm;"| <center>[http://appft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PG01&p=1&u=%2Fnetahtml%2FPTO%2Fsrchnum.html&r=1&f=G&l=50&s1=%2220020107184%22.PGNR.&OS=DN/20020107184&RS=DN/20020107184 US20020107184]</center>
| style=";padding:0.079cm;"| <center>8/8/2002</center>
| style=";padding:0.079cm;"| <center>None</center>
| style=";padding:0.079cm;"| <center>METHOD FOR TREATING MELANOMA </center>
| style=";padding:0.079cm;"| <center>The present invention discloses a method for treating patients having melanoma or melanoma associated symptoms by parenterally administering Product R, a peptide-nucleic acid preparation.</center>
| style=";padding:0.079cm;"| <center>Melanomas are usually treated by surgical excision, while patients with thick melanomas and those with regional or distant metastasis may benefit from other forms of therapy.Cytokines have been tested in the treatment of different skin cancers during the last decade, and treatment schedules have been established or proposed for several malignant skin tumors. Preferentially, the interferons and interleukin-2 were found to be effective in treating skin cancers including melanoma.But they were needed to be checked in combination with other products as they were anticipated to yield better results.</center>
| style=";padding:0.079cm;"| <center>The new method of treatment using the product R in combination with interferons not only sounded effectively but also proved to be an effective means .The administration is done in an sterile injectible form.</center>
 
|-
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''9'''</center>
| style=";padding:0.079cm;"| <center>[http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=4762705.PN.&OS=PN/4762705&RS=PN/4762705 US4762705] </center>
| style=";padding:0.079cm;"| <center>8/9/1988</center>
| style=";padding:0.079cm;"| <center>Schwimmer, Adolf W. | Schwartz, Irwin Steven | Rubin, David</center>
| style=";padding:0.079cm;"| <center>Cancer therapy with interferon </center>
| style=";padding:0.079cm;"| <center>The effectiveness of interferon for treatment against cancer may be increased by first administering an agent for inhibiting tyrosinase. In this manner the tyrosinase which is known to be produced by malignancies, and which may cause inactivation of the interferon, will be substantially inactivated prior to the interferon administration.</center>
| style=";padding:0.079cm;"| <center>Some of the the prior art patents doesn't trust on the use of interferons for treating all types of malignancies.The reason being the interferons are easily denatured in the enzymatic processes.So attempts were made out initially to find out the reasons for the denaturation even at high doses.Efforts were made to improve methods of cancer therapy using interferon.</center>
| style=";padding:0.079cm;"| <center>The solution has come out in the form of improved treatment method for treating cancer by the efforts of the present inventor.As the reason for the denaturation was found to be tyrosinase,attempts were made seriously to supress this tyrosinase.A composition was made finally with D-penicillamine that can suppress tyrosinase.</center>
 
|-
| style="background-color:#99ccff;;padding:0.079cm;"| <center>'''10'''</center>
| style=";padding:0.079cm;"| <center>[http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=5190751.PN.&OS=PN/5190751&RS=PN/5190751 US5190751] </center>
| style=";padding:0.079cm;"| <center>3/2/1993</center>
| style=";padding:0.079cm;"| <center>Schering Corporation</center>
| style=";padding:0.079cm;"| <center>Treatment of certain leukemias with a combination of gamma interferon and alpha interferon </center>
| style=";padding:0.079cm;"| <center>Human leukemia T-cells and B-cells are inhibited from proliferating by treatment with a combination of recombinant human alpha and gamma interferons, either simultaneously or sequentially, and the alpha interferon is preferably recombinant human alfa-2b interferon.</center>
| style=";padding:0.079cm;"| <center>The patent in the prior art posed a lot of problems with the use of gamma interferons alone in terms of the purity as the preparations previously were found to be contaminated.When used singly for the treatment of lekimias they were found to yield ineffective results.</center>
| style=";padding:0.079cm;"| <center>The solution was found to administer alpha and gamma interferons for the treatment of leukemias.It could inhibit the proliferation of susceptible leukemia cells with a cell proliferation inhibiting amount of a combination of both of the interferons.They are adminstered sequentially and simultaneously too to give good results.</center>
 
|}
==Taxonomy== [[Image:taxonomy melanoma mod1.jpg|700px|center|thumb| '''Taxonomy''']] == Sample Patents Analysis===*'''Patents:''' The above sample patents were analysed according to the taxonomy.
[[Media:Sample analysis of Treating of melanoma.xls| '''Click here to download Sample analysis sheet on Interferon for treatment of Melanomas''']]
 
* '''Scientific Literature:'''* [[Media:Article Analysis Of Melanoma.xls |'''Click here to download Melanoma Treatment Using IFN: sample articles]]
 
==Patent Ranking==
10 Sample Patents were ranked according to the patent focus.
*Patent Ranking Details
1 : Granted Patent & Focus in Independent Claim <br>
2 : Granted Patent & Focus in Dependent Claim <br>
3 : Published Patent & Focus in independent Claim <br>
4 : Published Patent & Focus in Dependent claim <br>
 
{|border="2" cellspacing="0" cellpadding="4" width="100%"
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>S.No</b></center>
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>Patent</b></center>
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>Type</b></center>
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>Patent Ranking</b></center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>1</b></center>
| style="padding:0.079cm;"| <center>US7482014B2</center>
| style="padding:0.079cm;"| <center>Granted And Independent Claim</center>
| style="padding:0.079cm;"| <center>1</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>2</b></center>
| style="padding:0.079cm;"| <center>US5997858A</center>
| style="padding:0.079cm;"| <center>Granted And Independent Claim</center>
| style="padding:0.079cm;"| <center>1</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>3</b></center>
| style="padding:0.079cm;"| <center>EP288055A1</center>
| style="padding:0.079cm;"| <center>Granted And Independent Claim</center>
| style="padding:0.079cm;"| <center>1</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>4</b></center>
| style="padding:0.079cm;"| <center>EP241242A1</center>
| style="padding:0.079cm;"| <center>Granted And Dependent Claim</center>
| style="padding:0.079cm;"| <center>2</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>5</b></center>
| style="padding:0.079cm;"| <center>US20100086518 </center>
| style="padding:0.079cm;"| <center>Published And Dependent</center>
| style="padding:0.079cm;"| <center>4</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>6</b></center>
| style="padding:0.079cm;"| <center>US4846782 </center>
| style="padding:0.079cm;"| <center>Granted And Dependent Claim</center>
| style="padding:0.079cm;"| <center>2</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>7</b></center>
| style="padding:0.079cm;"| <center>US5824300 </center>
| style="padding:0.079cm;"| <center>Granted And Dependent Claim</center>
| style="padding:0.079cm;"| <center>2</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>8</b></center>
| style="padding:0.079cm;"| <center>US20020107184</center>
| style="padding:0.079cm;"| <center>Published And Independent</center>
| style="padding:0.079cm;"| <center>3</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>9</b></center>
| style="padding:0.079cm;"| <center>US4762705 </center>
| style="padding:0.079cm;"| <center>Granted And Independent Claim</center>
| style="padding:0.079cm;"| <center>1</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center><b>10</b></center>
| style="padding:0.079cm;"| <center>US5190751 </center>
| style="padding:0.079cm;"| <center>Granted And Independent Claim</center>
| style="padding:0.079cm;"| <center>1</center>
 
|}
 
==Clinical Trials==
*'''Database:''' [http://clinicaltrials.gov/ '''Clinical trials''']
*'''Searched on:''' Feb 25th, 2011
*[[Media:clinical trials treatment of melanoma.xls |'''Please click here to download the clinical trial excel sheet''']]
==IP Activity Graphs Of Sample Patents==
* The geographical distribution is based on 10 sample patent numbers along with all their family members.
[[Image:Geographical Distribution based on Family members Melanoma 1.jpg|center|thumb|500 px| Geographical Distribution based on Family members Melanoma]]
 
==Market Report==
===Interferon types & Their Compositions===
{|border="2" cellspacing="0" cellpadding="4" width="100%"
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''S.No'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Generic Name'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Brand Name'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Company Name'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Composition'''</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''1'''</center>
| style="padding:0.079cm;"| <center>Alpha IFN</center>
| style="padding:0.079cm;"| <center>Intron®,Roferon®-A</center>
| style="padding:0.079cm;"| <center>Schering Corporation</center>
| style="padding:0.079cm;"| <center>Active Ingredient-Interferon alfa-2aInactive Ingredients- sodium chloride, ammonium acetate, polysorbate 80, glycine, sodium phosphate dibasic,sodium phosphate monobasic, human albumin, preservative: benzyl alcohol.</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''2'''</center>
| style="padding:0.079cm;"| <center>Beta IFN</center>
| style="padding:0.079cm;"| <center>Avonex</center>
| style="padding:0.079cm;"| <center>Biogen IDEC</center>
| style="padding:0.079cm;"| <center>Active Ingredient-Beta interferon,Inactive Ingredients-65 to 90 wt % of polyol,and a p-hydroxybenzoate,carboxymethyl cellulose,human serum albumin</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''3'''</center>
| style="padding:0.079cm;"| <center>Gamma IFN</center>
| style="padding:0.079cm;"| <center>Actimmune®</center>
| style="padding:0.079cm;"| <center>Intermune</center>
| style="padding:0.079cm;"| <center>Active Ingredient-interferon gamma-1b.,Inactive Ingredients-Polyethylene Glycol,dextran ,hydroxyethylstarch </center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''4'''</center>
| style="padding:0.079cm;"| <center>Pegylated IFN</center>
| style="padding:0.079cm;"| <center>Peg Intron</center>
| style="padding:0.079cm;"| <center>Schering-Plough</center>
| style="padding:0.079cm;"| <center>Active ingredient-peginterferon alfa-2b,Inactive ingredients: dibasic sodium phosphate anhydrous, monobasicsodium phosphate dihydrate, sucrose, polysorbate 80.</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''5'''</center>
| style="padding:0.079cm;"| <center>Recombinant IFN</center>
| style="padding:0.079cm;"| <center>(Rebetron®, Rebetol®).</center>
| style="padding:0.079cm;"| <center>Schering Corporation</center>
| style="padding:0.079cm;"| <center>Active Ingredient-Ribavirin,Inactive Ingredients-microcrystalline cellulose, lactose monohydrate, croscarmellose sodium,sodium phosphate dibasic and sodium phosphate dibasic and sodium phosphate monobasic as buffering agents;human albumin as a stabilizer.</center>
 
|}
 
===Interferon Types & Description Of Products===
{|border="2" cellspacing="0" cellpadding="4" width="100%"
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''S.No'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Company Name'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Product'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Description'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Source'''</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''1'''</center>
| style="padding:0.079cm;"| <center>Schering Corporation</center>
| style="padding:0.079cm;"| <center>Intron®,Roferon®-A</center>
| style="padding:0.079cm;"| <center>Intron A is an interferon, a group of naturally occurring proteins that were first discovered as a result of their ability to prevent viral replication. Intron A is marketed in 72 countries worldwide for as many as 16 indications.In the United States it has been cleared for use by the FDA for chronic viral hepatitis B, chronic viral hepatitis C, malignant melanoma, hairy cell leukemia, AIDS-related Kaposi’s sarcoma and condylomata acuminata (venereal warts).INTRON A recombinant for Injection has been classified as an alpha interfero nand is a water-soluble protein with a molecular weight of 19,271 daltons produced by recombinant DNA techniques. It is obtained from the bacterial fermentation of a strain of Escherichia coli bearing a genetically engineered plasmid containing an interferon alfa- 2b gene from human leukocytes. The fermentation is carried out in a defined nutrient medium containing the antibiotic tetracycline hydrochloride at a concentration of 5 to 10 mg/L; the presence of this antibiotic is not detectable in the final product. The specific activity of interferon alfa-2b, recombinant is approximately 2.6 x 108 IU/mg protein as measured by the HPLC assay.</center>
| style="padding:0.079cm;"| <center>[http://www.introna.com/maintenance.html http://www.introna.com/maintenance.html]</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''2'''</center>
| style="padding:0.079cm;"| <center>Biogen IDEC</center>
| style="padding:0.079cm;"| <center>Avonex</center>
| style="padding:0.079cm;"| <center>Avonex, manufactured by Biogen, is a form of beta interferon (interferon beta, IFN-b) used to modify the course of multiple sclerosis. While not a cure, Avonex has been shown in clinical trials to reduce the average relapse rate in people with the relapsing-remitting multiple sclerosis form of the disease. It is identical to the naturally occurring protein found in the human body. It is manufactured by extracting the drug from Chinese hamster ovary cells. Avonex is the same substance as Rebif but administered differently (30 mcg, intra-muscularly, once a week as against 22 mcg or 44 mcg, sub-cutaneously, 3 times a week for Rebif). Avonex is usually given in the large muscles of the thigh, upper arm, or hip.</center>
| style="padding:0.079cm;"| <center>[http://www.mult-sclerosis.org/Avonex.html http://www.mult-sclerosis.org/Avonex.html]</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''3'''</center>
| style="padding:0.079cm;"| <center>Intermune</center>
| style="padding:0.079cm;"| <center>Actimmune®</center>
| style="padding:0.079cm;"| <center>Actimmune(R) is a synthesized version of interferon gamma, a naturally occurring protein believed to stimulate the immune system. InterMune markets Actimmune(R) for the treatment of two life-threatening congenital diseases: chronic granulomatous disease and severe, malignant osteopetrosis. The most common side effects are flu-like symptoms, including headache, fatigue, fever, chills, and rash. InterMune was granted two composition-of-matter patents related to interferon gamma-1b in the United States, extending its patent protection until 2022.</center>
| style="padding:0.079cm;"| <center>[http://www.actimmune.com/ http://www.actimmune.com/]</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''4'''</center>
| style="padding:0.079cm;"| <center>Schering-Plough</center>
| style="padding:0.079cm;"| <center>Peg Intron</center>
| style="padding:0.079cm;"| <center>Peg-Intron (peginterferon alfa-2b) Powder for Injection has been approved by the FDA.Peg-Intron is a longer-acting formulation of Schering-Plough's Intron A, which is a recombinant version of a naturally occurring alpha interferon. In contrast to Intron A, which is administered three times weekly, Peg-Intron is administered subcutaneously once a week. This reduced frequency of administration may increase patient compliance.</center>
| style="padding:0.079cm;"| <center>[http://www.pegintron.com/index.html http://www.pegintron.com/index.html]</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''5'''</center>
| style="padding:0.079cm;"| <center>Schering Corporation</center>
| style="padding:0.079cm;"| <center>(Rebetron®, Rebetol®).</center>
| style="padding:0.079cm;"| <center>REBETOL is a medicine used with either interferon alfa-2b (Intron A) or peginterferon alfa-2b (PegIntron) to treat chronic (lasting a long time) hepatitis C infection in people 3 years and older with liver disease.REBETOL Capsules consist of a white powder in a white, opaque, gelatin capsule. Each capsule contains 200 mg ribavirin and the inactive ingredients microcrystalline cellulose, lactose monohydrate, croscarmellose sodium, and magnesium stearate. The capsule shell consists of gelatin, sodium lauryl sulfate, silicon dioxide, and titanium dioxide. The capsule is printed with edible blue pharmaceutical ink which is made of shellac, anhydrous ethyl alcohol, isopropyl alcohol, n-butyl alcohol, propylene glycol, ammonium hydroxide, and FD&C Blue #2 aluminum lake.</center>
| style="padding:0.079cm;"| <center>[http://www.merck.com/product/home.html http://www.merck.com/product/home.html]</center>
 
|}
 
 
===Global Revenue Data Of products===
{|border="2" cellspacing="0" cellpadding="4" width="100%"
|bgcolor = "#99ccff" rowspan = "2"|'''S.No'''
|bgcolor = "#99ccff" rowspan = "2"|''' Generic Name'''
|bgcolor = "#99ccff" rowspan = "2"|''' Brand Name'''
|bgcolor = "#99ccff" rowspan = "2"|''' Company'''
|bgcolor = "#99ccff" colspan = "3"|''' Global revenue ($ Million )'''
|-
|align = "right" bgcolor = "#C5D9F1"|'''2008'''
|align = "right" bgcolor = "#C5D9F1"|'''2009'''
|align = "right" bgcolor = "#C5D9F1"|'''2010'''
|-
|bgcolor = "#99ccff"|'''1'''
| Alpha IFN
| Intron®,Roferon®-A
|Schering Corporation
|align = "right"|
|align = "right"| 38.4 2
|align = "right"|
|-
|bgcolor = "#99ccff"|'''2'''
| Beta IFN
| Avonex
|Biogen IDEC
|align = "right"|2518.4
|align = "right"|2322.9
|align = "right"| 2202.6 3
|-
|bgcolor = "#99ccff"|'''3'''
| Gamma IFN
| Actimmune®
| Intermune
|align = "right"|29880
|align = "right"| 25428 4
|align = "right"|
|-
|bgcolor = "#99ccff"|'''4'''
| Pegylated IFN
| Peg Intron
| Schering-Plough
|align = "right"|
|align = "right"| 148.7 5
|align = "right"|
|-
|bgcolor = "#99ccff"|'''5'''
| Recombinant IFN
|Rebetron®, Rebetol®
| Schering Corporation
|align = "right"|
|align = "right"|36.1
|align = "right"|
|-
|}
 
==Biosimilars Of Interferons==
 
Biosimilar interferons are the major drug class in the recombinant non-glycosylated proteins market due to their extensive use in the treatment of various genetic and environmental disorders. The overall biosimilar market for interferons is categorized into the submarkets for alpha, beta, and gamma interferons, all of which are used extensively in the treatment of various conditions such as lymphoma, hairy cell leukemia, and multiple sclerosis.
 
While the interferon market growth may be inhibited by the side effects of each of its three drug categories, the market presents many opportunities to new entrants as only a few players currently operate in this relatively unfragmented market.
 
The global recombinant interferon market stood at $75.3 million in 2008 and is expected to reach $3.9 billion by 2014 at a CAGR of 82.9% from 2009 to 2014. The American biosimilar interferons market is expected to attain a market worth $1.5 billion by 2014 at a CAGR of 91.5%.[http://goliath.ecnext.com/coms2/gi_0198-669040/4-Biosimilar-products.html Biosimilars ; Global Market]
 
 
{|border="2" cellspacing="0" cellpadding="4" width="100%"
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''S.No'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Product'''</center>
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''Global market For Biosimilars'''</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''1'''</center>
| style="padding:0.079cm;"| <center>Interferon Alfa</center>
| style="padding:0.079cm;"| <center>The global market for biosimilar interferon Alfa was $36.7 million in 2008 and is expected to reach $1.5 billion in 2014 at a CAGR of 76.5% from 2009 to 2014. While Asian market for biosimilar Alfa interferons commanded the highest share in 2008 with $17.5 million, the American market is expected to have the highest CAGR of 88.3% from 2009 to 2014.The world's top two branded Interferon products generated sales of $1,510 million and $910 million each in 2008. The blockbuster sales of innovative Interferon Alfa products thus present encouragement for biosimilar Interferon Alfa manufacturers[http://goliath.ecnext.com/coms2/gi_0198-669040/4-Biosimilar-products.html data].</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''2'''</center>
| style="padding:0.079cm;"| <center>Interferon beta</center>
| style="padding:0.079cm;"| <center>The global biosimilar interferon beta-1a market is estimated to grow from $36.3 million in 2008 to $2.2 billion by 2014 at a CAGR of 87.8% from 2009 to 2014. However, the U.S. and Europe sales of branded interferon-betas are expected to fall from $4.6 billion in 2010 to $2.4 billion in 2017. The soaring cost of clinical development, the conservative prescribing habits of neurologists, and the expected decline in the use of interferon-betas may induce biosimilar developers to explore other classes of biologics to invest their R&D funds[http://goliath.ecnext.com/coms2/gi_0198-669040/4-Biosimilar-products.html data].</center>
 
|-
| style="background-color:#99ccff;padding:0.079cm;"| <center>'''3'''</center>
| style="padding:0.079cm;"| <center>Interferon gamma</center>
| style="padding:0.079cm;"| <center>The global biosimilar interferon gamma market was $2.2 million 2008 and is expected to reach $141.5 million in 2014 at a CAGR of 94.2% from 2009 to 2014. While the Asian market accounted for the highest share of $0.5 million in 2008, the American market is expected to have the highest CAGR of 107.6% from 2009 to 2014[http://goliath.ecnext.com/coms2/gi_0198-669040/4-Biosimilar-products.html data].</center>
 
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