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Riga 1: {{Disclaimer\|medico}} ~~{{S\|farmaci\|medicina}}~~ {{Composto chimico ~~{{Disclaimer medico}}~~ ~~{{Farmaco~~ \| nome_IUPAC = \| ~~immagine~~immagine1_nome = \| immagine1_dimensioni = ~~\| dimensione_immagine =~~ \| ~~immagine2~~immagine2_nome = \| immagine2_dimensioni = ~~\| dimensione_immagine2 =~~ ~~\| numero_CAS = 615258-40-7~~ \| prefisso_ATC = M05 \| suffisso_ATC = BX04 Riga 13 ⟶ 11: \| DrugBank = \| formula = C<sub>6404</sub>H<sub>9912</sub>N<sub>1724</sub>O<sub>2004</sub>S<sub>50</sub> \| massa_molecolare = 144.7 [[kDa]] \| smiles = \| ~~sinonimi~~nomi_alternativi = \| densità_condensato = ~~\| densità =~~ \| temperatura_di_fusione = ~~\| punto_di_fusione = ° C~~ \| temperatura_di_ebollizione = ~~\| punto_di_ebollizione = ° C~~ \| ~~solubilità~~solubilità_acqua = \| potere_rotatorio_specifico = ~~\| potere_rotatorio =~~ \| entalpia_standard_combustione = \| biodisponibilità = Riga 27 ⟶ 25: \| categoria = \| teratogenesi = ~~\| fascia = Fascia~~ ~~\| dispensazione =~~ \| somministrazione = Sottocutanea (ogni 6 mesi) }} [[File:Denosumab.jpg\|thumb\|Denosumab]] Il '''denosumab''', commercializzato con i nomi ''Prolia'' e ''Xgeva'', è un [[anticorpo monoclonale]] completamente [[anticorpo umanizzato\|umanizzato]] indicato per il trattamento dell'[[osteoporosi]] post-menopausale (PMO), il rimaneggiamento con perdita di massa ossea per [[artrite reumatoide]] (AR) o [[metastasi]] ossee e per contrastare le lesioni osteolitiche da [[mieloma multiplo]].<ref name="pmid16495394">{{Cita pubblicazione \| autore = McClung MR, Lewiecki EM, Cohen SB, ''et al.'' \|titolo = Denosumab in postmenopausal women with low bone mineral density \| rivista = N. Engl. J. Med. \| volume = 354 \| numero = 8 \| pagine = 821–31 \| anno = 2006 \| mese=febbraio\| pmid = 16495394 \| doi = 10.1056/NEJMoa044459 }}</ref><ref name="Ellis-2008">{{Cita pubblicazione \| cognome = Ellis \| nome = GK. \| coautori = HG. Bone; R. Chlebowski; D. Paul; S. Spadafora; J. Smith; M. Fan; S. Jun \| titolo = Randomized trial of denosumab in patients receiving adjuvant aromatase inhibitors for nonmetastatic breast cancer. \| rivista = J Clin Oncol \| volume = 26 \| numero = 30 \| pagine = 4875-82 \| mese=ottobre\| anno = 2008 \| doi = 10.1200/JCO.2008.16.3832 \| pmid = 18725648 }}</ref> ==Meccanismo d'azione== Il '''denosumab''', nome commerciale ''Prolia'' e ''Xgeva'', è un anticorpo monoclonale completamente umano indicato per il trattamento dell'osteoporosi post-menopausale (PMO) e la distruzione delle ossa a causa di artrite reumatoide (AR) o tumori metastatici.<ref name="pmid16495394">{{cite journal \| author = McClung MR, Lewiecki EM, Cohen SB, ''et al.'' \|title = Denosumab in postmenopausal women with low bone mineral density \| journal = N. Engl. J. Med. \| volume = 354 \| issue = 8 \| pages = 821–31 \| year = 2006 \| month = February \| id = PMID 16495394 \| doi = 10.1056/NEJMoa044459 \| url = \| issn = }}</ref><ref name="Ellis-2008">{{Cita pubblicazione \| cognome = Ellis \| nome = GK. \| coauthors = HG. Bone; R. Chlebowski; D. Paul; S. Spadafora; J. Smith; M. Fan; S. Jun \| titolo = Randomized trial of denosumab in patients receiving adjuvant aromatase inhibitors for nonmetastatic breast cancer. \| rivista = J Clin Oncol \| volume = 26 \| numero = 30 \| pagine = 4875-82 \| mese = Oct \| anno = 2008 \| doi = 10.1200/JCO.2008.16.3832 \|id = PMID 18725648 }}</ref> Il denosumab agisce formando degli [[immunocomplessi]] con il [[RANKL]] (RANK Ligand), proteina che agisce come segnale primario nella promozione della rimozione ossea legandosi al recettore [[RANK]]. In numerose condizioni caratterizzate da perdita di massa ossea vi è uno squilibrio tra il RANKL (attivatore [[osteoclasti]]co) che risulta aumentato e l'[[osteoprotegerina]] (inibitore osteoclastico). Studi clinici hanno dimostrato che il denosumab possiede un profilo di sicurezza simile ai [[bisfosfonati]] e che può essere altrettanto o più efficace dei bifosfonati nel prevenire la perdita ossea causata da {{abbr\|PMO\|osteoporosi post-menopausale}}, {{abbr\|AR\|artrite reumatoide}}, o durante il trattamento delle metastasi ossee.<ref name="urlLandes Bioscience Journals: mAbs">{{Cita web \| url = http://www.landesbioscience.com/journals/mabs/article/8592/ \| titolo = Landes Bioscience Journals: mAbs \| autore = \| data = \| lingua = en \| accesso = }}</ref> Il denosumab agisce come un attivatore anti-recettore del fattore nucleare ([[NF-kB]]) ([[RANK]]) [[ligando]] umano. Il target RANKL (RANK ligand) è una proteina che agisce come segnale primario nella promozione della rimozione ossea. In molte condizioni in cuoi vi è una perdita ossea, RANKL travolge la naturale difesa del organismo contro la perdita ossea. Il farmaco è stato sviluppato dalla ''Amgen'', con il nome ''Prolia'', dal giugno 2010,<ref name="urlFDA clears Amgens bone-strengthening drug Prolia \| Bioscience Technology Online">{{Cita web \| url = http://www.biosciencetechnology.com/News/FeedsAP/2010/06/fda-clears-amgens-bone-strengthening-drug-prolia/ \| titolo = FDA clears Amgens bone-strengthening drug Prolia \| Bioscience Technology Online \| autore = \| data = \| lingua = en \| accesso = \| urlmorto = sì \| urlarchivio = https://archive.is/20120723192347/http://www.biosciencetechnology.com/News/FeedsAP/2010/06/fda-clears-amgens-bone-strengthening-drug-prolia/ \| dataarchivio = 23 luglio 2012 }}</ref><ref name="urlMedical News: FDA Approves Denosumab for Osteoporosis - in Endocrinology, Osteoporosis from MedPage Today">{{Cita web \| url = http://www.medpagetoday.com/Endocrinology/Osteoporosis/20432 \| titolo = Medical News: FDA Approves Denosumab for Osteoporosis - in Endocrinology, Osteoporosis from MedPage Today \| autore = \| data = \| lingua = en \| accesso = }}</ref> per il trattamento dell'osteoporosi (PMO), mentre per il trattamento delle [[metastasi]] ossee, con il nome ''Xgeva'', dal novembre 2010.<ref name="urlGEN \| News Highlights: Amgen's Denosumab Cleared by FDA for Second Indication">{{Cita web \| url = http://www.genengnews.com/gen-news-highlights/amgen-s-denosumab-cleared-by-fda-for-second-indication/81244270/ \| titolo = GEN \| News Highlights: Amgen's Denosumab Cleared by FDA for Second Indication \| autore = \| data = \| lingua = en \| accesso = \| dataarchivio = 7 aprile 2018 \| urlarchivio = https://web.archive.org/web/20180407054018/https://www.genengnews.com/gen-news-highlights/amgen-s-denosumab-cleared-by-fda-for-second-indication/81244270/ \| urlmorto = sì }}</ref> Studi clinici hanno dimostrato che denosumab possiede un profilo di sicurezza simile a [[bisfosfonati]]e che può essere altrettanto o più efficaci di bifosfonati nel prevenire la perdita ossea causata da PMO, RA, o durante il trattamento del cancro e delle metastasi ossee.<ref name="urlLandes Bioscience Journals: mAbs">{{cite web \| url = http://www.landesbioscience.com/journals/mabs/article/8592/ \| title = Landes Bioscience Journals: mAbs \| author = \| authorlink = \| coauthors = \| date = \| format = \| work = \| publisher = \| pages = \| language = en \| archiveurl = \| archivedate = \| quote = \| accessdate = }}</ref> Negli USA la Amgen stima ogni anno fatturati di circa 12,6 miliardi di $.<ref name="urlGEN \| News Highlights: Amgen's Denosumab Cleared by FDA for Second Indication"/> Il farmaco è stato sviluppato dalla ''Amgen'', con il nome ''Prolia'', dal giugno 2010,<ref name="urlFDA clears Amgens bone-strengthening drug Prolia \| Bioscience Technology Online">{{cite web \| url = http://www.biosciencetechnology.com/News/FeedsAP/2010/06/fda-clears-amgens-bone-strengthening-drug-prolia/ \| title = FDA clears Amgens bone-strengthening drug Prolia \| Bioscience Technology Online \| author = \| authorlink = \| coauthors = \| date = \| format = \| work = \| publisher = \| pages = \| language = en \| archiveurl = \| archivedate = \| quote = \| accessdate = }}</ref><ref name="urlMedical News: FDA Approves Denosumab for Osteoporosis - in Endocrinology, Osteoporosis from MedPage Today">{{cite web \| url = http://www.medpagetoday.com/Endocrinology/Osteoporosis/20432 \| title = Medical News: FDA Approves Denosumab for Osteoporosis - in Endocrinology, Osteoporosis from MedPage Today \| author = \| authorlink = \| coauthors = \| date = \| format = \| work = \| publisher = \| pages = \| language = en \| archiveurl = \| archivedate = \| quote = \| accessdate = }}</ref> per il trattamento dell'osteoporosi (PMO); mentre per il trattamento delle [[metastasi]] ossee, con il nome ''Xgeva'', dal novembre 2010.<ref name="urlGEN \| News Highlights: Amgenâ€™s Denosumab Cleared by FDA for Second Indication">{{cite web \| url = http://www.genengnews.com/gen-news-highlights/amgen-s-denosumab-cleared-by-fda-for-second-indication/81244270/ \| title = GEN \| News Highlights: Amgenâ€™s Denosumab Cleared by FDA for Second Indication \| author = \| authorlink = \| coauthors = \| date = \| format = \| work = \| publisher = \| pages = \| language = en \| archiveurl = \| archivedate = \| quote = \| accessdate = }}</ref> Altre ricerche sono in corso per nuove indicazioni. ==Indicazioni terapeutiche== Gli effetti collaterali più frequenti sono: dolore alla schiena, iper-colesterolemia, infezioni vescicali.<ref name="urlFDA clears Amgens bone-strengthening drug Prolia \| Bioscience Technology Online">{{cite web \| url = http://www.biosciencetechnology.com/News/FeedsAP/2010/06/fda-clears-amgens-bone-strengthening-drug-prolia/ \| title = FDA clears Amgens bone-strengthening drug Prolia \| Bioscience Technology Online \| author = \| authorlink = \| coauthors = \| date = \| format = \| work = \| publisher = \| pages = \| language = en \| archiveurl = \| archivedate = \| quote = \| accessdate = }}</ref> Gli effetti collaterali più gravi sono: ipocalcemia, infezioni gravi comprese le infezioni cutanee, dermatiti eczema e rashes.<ref name="urlMedical News: FDA Approves Denosumab for Osteoporosis - in Endocrinology, Osteoporosis from MedPage Today">{{cite web \| url = http://www.medpagetoday.com/Endocrinology/Osteoporosis/20432 \| title = Medical News: FDA Approves Denosumab for Osteoporosis - in Endocrinology, Osteoporosis from MedPage Today \| author = \| authorlink = \| coauthors = \| date = \| format = \| work = \| publisher = \| pages = \| language = en \| archiveurl = \| archivedate = \| quote = \| accessdate = }}</ref> Denosumab è indicato per<ref>{{cita web\|url=https://www.cancer.gov/about-cancer/treatment/drugs/denosumab\|titolo=FDA: Denosumab\|accesso=6 luglio 2021\|lingua=en}}</ref> * aumentare la massa ossea in donne ad alto rischio di [[frattura (medicina)\|frattura]] che ricevono [[terapia adiuvante]] con [[inibitori dell'aromatasi]] per il [[tumore della mammella]]; * aumentare la massa ossea negli uomini che sono ad alto rischio di frattura e sono sottoposti a [[terapia di deprivazione androgenica]] del [[cancro alla prostata]] non metastatico. * la prevenzione delle fratture ossee in malati di [[mieloma multiplo]] e tumori metastatizzati alle ossa * la terapia dell'[[osteoclastoma]] * il trattamento dell'[[ipercalcemia]] oncologica ==Effetti collaterali== Gli effetti collaterali più frequenti sono: [[iper-colesterolemia]], [[Infezione delle vie urinarie\|infezioni vescicali]]<ref name="urlFDA clears Amgens bone-strengthening drug Prolia \| Bioscience Technology Online"/>, [[ipocalcemia]], [[infezioni]] gravi comprese le infezioni cutanee, [[dermatiti]], [[eczema]] e rash cutaneo<ref name="urlMedical News: FDA Approves Denosumab for Osteoporosis - in Endocrinology, Osteoporosis from MedPage Today"/>, [[osteonecrosi]] della [[mandibola]]/[[mascella]]. L'induzione di ipocalcemia potrebbe essere utilizzata in caso di [[ipercalcemia]] maligna. Negli USA la Amgen stima ogni anno fatturati di circa 12,6 bilioni di $.<ref name="urlGEN \| News Highlights: Amgenâ€™s Denosumab Cleared by FDA for Second Indication">{{cite web \| url = http://www.genengnews.com/gen-news-highlights/amgen-s-denosumab-cleared-by-fda-for-second-indication/81244270/ \| title = GEN \| News Highlights: Amgenâ€™s Denosumab Cleared by FDA for Second Indication \| author = \| authorlink = \| coauthors = \| date = \| format = \| work = \| publisher = \| pages = \| language = en \| archiveurl = \| archivedate = \| quote = \| accessdate = }}</ref> == Note == <references/> == Bibliografia == * {{~~cite~~Cita ~~book~~libro\|~~author~~autore=Frank Ashall\|~~title~~titolo=Le grandi scoperte scientifiche\|url=http://books.google.com/books?id=GXsecqAh6MEC&pg=PA245\|~~accessdate=\|year~~anno=1999\|~~publisher~~editore=Armando Editore\|~~isbn~~pagine=~~9788871449494~~245–\|~~pages~~isbn=~~245–~~978-88-7144-949-4}} * {{~~cite~~Cita ~~book~~libro\|~~author1~~autore=Abul K. Abbas\|~~author2~~autore2=Andrew H. Lichtman\|~~author3~~autore3=Shiv Pillai\|~~title~~titolo=Immunologia cellulare e molecolare\|url=http://books.google.com/books?id=9SFm3nMO_gUC&pg=PA79\|~~accessdate= \|year~~anno=2010\|~~publisher~~editore=Elsevier srl\|~~isbn~~pagine=~~9788821431760~~79–\|~~pages~~isbn=~~79–~~978-88-214-3176-0}} * {{~~cite~~Cita ~~book~~libro\|~~author1~~autore=Abul K. Abbas\|~~author2~~autore2=Andrew H. Lichtman\|~~title~~titolo=Le basi dell'immunologia\|url=http://books.google.com/books?id=szHkdI9buskC&pg=PA70\|~~accessdate\|year~~anno=2006\|~~publisher~~editore=Elsevier srl\|~~isbn~~pagine=~~9788885675858~~70–\|~~pages~~isbn=~~70–~~978-88-85675-85-8}} * {{~~cite~~Cita ~~book~~libro\|~~author1~~autore=Humphrey P. Rang\|~~author2~~autore2=M. Maureen Dale\|~~author3~~autore3=James M. Ritter\|~~title~~titolo=Farmacologia\|url=http://books.google.com/books?id=HGcP_ip4SmgC&pg=PA778\|~~accessdate\|year~~anno=2008\|~~publisher~~editore=Elsevier srl\|~~isbn~~pagine=~~9788821430237~~778–\|~~pages~~isbn=~~778–~~978-88-214-3023-7}} * {{~~cite~~Cita ~~book~~libro\|~~author~~autore=Enzo Fagiolo\|~~title~~titolo=Immunoematologia\|url=http://books.google.com/books?id=ErRtMU7SKhkC&pg=PA16\|~~accessdate=\|year~~anno=2007\|~~publisher~~editore=Mediserve s.r.l.\|~~isbn~~pagine=~~9788882041359~~16–\|~~pages~~isbn=~~16–~~978-88-8204-135-9}} * {{~~cite~~Cita ~~book~~libro\|~~author~~autore=Paolo Larizza\|~~title~~titolo=Trattato di medicina interna\|url=http://books.google.com/books?id=Rt4_C55_Ls4C&pg=PA909\|~~accessdate=\|year~~anno=2005\|~~publisher~~editore=PICCIN\|~~isbn~~pagine=~~9788829917211~~909–\|~~pages~~isbn=~~909–~~978-88-299-1721-1}} * {{~~cite~~Cita ~~book~~libro\|~~author~~autore=Angelo Sghirlanzoni\|~~title~~titolo=Terapia Delle Malattie Neurologiche\|url=http://books.google.com/books?id=LCNUGXlL4FQC&pg=PA113\|~~accessdate= \|date~~data=3 ~~April~~aprile 2010\|~~publisher~~editore=Springer\|~~isbn~~pagine=~~9788847011199~~113–\|~~pages~~isbn=~~113–~~978-88-470-1119-9}} * {{~~cite~~Cita ~~book~~libro\|~~author~~autore=Thomas C. King\|~~title~~titolo=Patologia\|url=http://books.google.com/books?id=1CgV-Td_I3oC&pg=PA156\|~~accessdate= \|year~~anno=2008\|~~publisher~~editore=Elsevier srl\|~~isbn~~pagine=~~9788821430190~~156–\|~~pages~~isbn=~~156–~~978-88-214-3019-0}} * {{~~cite~~Cita web \| url = http://whqlibdoc.who.int/druginfo/INN_2000_list43.pdf WHO-Lista INN degli Anticorpi monoclonali\| ~~title~~titolo = whqlibdoc.who.int \| ~~author~~autore = \| ~~authorlink~~data = \| ~~coauthors~~lingua = en\| ~~date~~accesso =\|~~format~~ ~~= \| work~~urlmorto = sì\| ~~publisher~~urlarchivio = https://web.archive.org/web/20091016235049/http://whqlibdoc.who.int/druginfo/INN_2000_list43.pdf\| ~~pages~~dataarchivio =16 ~~\| language = en \| archiveurl = \| archivedate = \| quote =\| accessdate =~~ottobre 2009}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author~~autore=Marie A. Simmons\|~~title~~titolo=Monoclonal antibodies: new research\|url=http://books.google.com/books?id=jxhKskARw6IC\|~~accessdate=\|year~~anno=2005\|~~publisher~~editore=Nova Publishers\|isbn=~~9781594542473~~978-1-59454-247-3\|lingua=en}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author~~autore=Zhiqiang An\|~~title~~titolo=Therapeutic Monoclonal Antibodies: From Bench to Clinic\|url=http://books.google.com/books?id=agdx2rtK7E0C\|~~accessdate= \|date~~data=8 ~~September~~settembre 2009\|~~publisher~~editore=John Wiley and Sons\|isbn=~~9780470117910~~978-0-470-11791-0\|lingua=en}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author~~autore=James W. Goding\|~~title~~titolo=Monoclonal antibodies: principles and practice : production and application of monoclonal antibodies in cell biology, biochemistry and immunology\|url=http://books.google.com/books?id=jPk4ZY4CnQQC\|~~accessdate=\|year~~anno=1996\|~~publisher~~editore=Academic Press\|isbn=~~9780122870231~~978-0-12-287023-1\|lingua=en}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author~~autore=Steve Shire\|~~title~~titolo=Current Trends in Monoclonal Antibody Development and Manufacturing\|url=http://books.google.com/books?id=YTbJpdPhgT4C\|~~accessdate~~data= ~~\|date=April~~aprile 2009\|~~publisher~~editore=Springer\|isbn=~~9780387766423~~978-0-387-76642-3\|lingua=en}} === Denosumab === * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author~~autore=G. David Roodman\|~~title~~titolo=Myeloma Bone Disease\|url=http://books.google.com/books?id=cp1NBe2ob00C&pg=PA177\|~~accessdate= \|date~~data=4 ~~May~~maggio 2010\|~~publisher~~editore=Springer\|pagine=177–\|isbn=~~9781607615538~~978-1-60761-553-8\|~~pages~~lingua=~~177–~~en}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author~~autore=Yongwon Choi\|~~title~~titolo=Osteoimmunology: Interactions of the Immune and Skeletal Systems II\|url=http://books.google.com/books?id=B9KVFiJCc9kC&pg=PA89\|~~accessdate= \|date~~data=15 ~~November~~novembre 2009\|~~publisher~~editore=Springer\|pagine=89–\|isbn=~~9781441910493~~978-1-4419-1049-3\|~~pages~~lingua=~~89–~~en}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author1~~autore=Bruce A. Chabner\|~~author2~~autore2=Dan L. Longo\|~~title~~titolo=Cancer Chemotherapy and Biotherapy: Principles and Practice\|url=http://books.google.com/books?id=WL4arNFsQa8C&pg=PA735\|~~accessdate= \|date~~data=8 ~~November~~novembre 2010\|~~publisher~~editore=Lippincott Williams & Wilkins\|pagine=735–\|isbn=~~9781605474311~~978-1-60547-431-1\|~~pages~~lingua=~~735–~~en}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author1~~autore=William D. Figg\|~~author2~~autore2=Cindy H. Chau\|~~author3~~autore3=Eric J. Small\|~~title~~titolo=Drug Management of Prostate Cancer\|url=http://books.google.com/books?id=4KDrjeWA5-UC&pg=PA273\|~~accessdate= \|date~~data=1º ~~August~~agosto 2010\|~~publisher~~editore=Springer\|pagine=273–\|isbn=~~9781603278317~~978-1-60327-831-7\|~~pages~~lingua=~~273–~~en}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author~~autore=Harvard Health Publications\|~~title~~titolo=2010 Annual Report on Prostate Diseases\|url=http://books.google.com/books?id=5Y4Qun5z7_cC&pg=PA11\|~~accessdate= \|publisher~~editore=Harvard Health Publications\|pagine=11–\|isbn=~~9781935555223~~978-1-935555-22-3\|~~pages~~lingua=~~11–~~en}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author~~autore=Manfred Kaufmann\|~~title~~titolo=Management of Breast Diseases\|url=http://books.google.com/books?id=nsUBW3-qJ9MC&pg=PA369\|~~accessdate=\|date~~data=June 2009\|~~publisher~~editore=Springer\|pagine=369–\|isbn=~~9783540697428~~978-3-540-69742-8\|~~pages~~lingua=~~369–~~en}} * {{~~en}}{{cite~~Cita ~~book~~libro\|~~author~~autore=Zhiqiang An\|~~title~~titolo=Therapeutic Monoclonal Antibodies: From Bench to Clinic\|url=http://books.google.com/books?id=agdx2rtK7E0C&pg=PA138\|~~accessdate= \|date~~data=8 ~~September~~settembre 2009\|~~publisher~~editore=John Wiley and Sons\|pagine=138–\|isbn=~~9780470117910~~978-0-470-11791-0\|~~pages~~lingua=~~138–~~en}} == Voci correlate == * [[Anticorpi monoclonali ~~(lista)~~approvati per uso clinico]] * [[Nomenclatura degli anticorpi monoclonali]] * [[Anticorpi monoclonali (terapia)]] * [[Terapia con anticorpi monoclonali]] * [[Anticorpi monoclonali (nomenclatura)]] * [[Anticorpi monoclonali (uso clinico approvato)]] == ~~Collegamenti~~Altri ~~esterni~~progetti == {{interprogetto}} * {{Anticorpi monoclonali per il sistema immune}} ~~{{Navbox~~ ~~\| name =~~ {{Anticorpi monoclonali per ~~il sistema immune~~i tumori}} {{Controllo di autorità}} ~~\| title = [[Anticorpi monoclonali]] per il [[sistema immune]]~~ {{Portale\|chimica\|medicina}} ~~\| groupstyle = background-color: LightGreen~~ ~~\| group1 = [[Sistema immune]]<br /> ("-l(i[m])-")~~ ~~\| list1 = {{Navbox subgroup~~ ~~\| group1 = Umani<br /> ("-limu-")~~ \| list1 = ''[[immunosuppressione]]'': [[Adalimumab]] • [[Atorolimumab]] • [[Fresolimumab]] • [[Golimumab]] • [[Lerdelimumab]] • [[Metelimumab]] • [[Morolimumab]] ~~''Attivazione immunitaria'': [[Ipilimumab]] • [[Tremelimumab]]~~ ~~''Altri'': [[Bertilimumab]] • [[Zanolimumab]]~~ ~~\| group2 = Topo<br /> ("-limo-")~~ \| list2 = [[Afelimomab]] • [[Elsilimomab]] • [[Faralimomab]] • [[Gavilimomab]] • [[Inolimomab]] • [[Maslimomab]] • [[Nerelimomab]] • [[Odulimomab]] • [[Telimomab aritox]] • [[Vepalimomab]] • [[Zolimomab aritox]] ~~\| group3 = [[Anticorpo chimerico\|Chimerici]]<br /> ("-lixi-")~~ \| list3 = [[Basiliximab]] • [[Clenoliximab]] • [[Galiximab]] • [[Gomiliximab]] • [[Infliximab]] • [[Keliximab]] • [[Lumiliximab]] • [[Priliximab]] • [[Teneliximab]] • [[Vapaliximab]] ~~\| group4 = [[Anticorpo umanizzato\|Umanizzato]]<br /> ("-lizu-")~~ \| list4 = ''immunosuppressive:'' [[Aselizumab]] • [[Apolizumab]] • [[Benralizumab]]<sup>†</sup> • [[Cedelizumab]] • [[Certolizumab pegol]] • [[Daclizumab]] • [[Eculizumab]] • [[Efalizumab]] • [[Epratuzumab]] • [[Erlizumab]] • [[Fontolizumab]] • [[Mepolizumab]] • [[Natalizumab]] • [[Ocrelizumab]] • [[Omalizumab]] • [[Pascolizumab]] • [[Pexelizumab]] • [[PRO 140]]<sup>†</sup> • [[Reslizumab]] • [[Rontalizumab]] • [[Rovelizumab]] • [[Ruplizumab]] • [[Siplizumab]] • [[Talizumab]] • [[Teplizumab]] • [[Tocilizumab]] • [[Toralizumab]] • [[Vedolizumab]] • [[Visilizumab]] • [[TGN1412]]<sup>§</sup><br/>''non-immunosuppressive:''[[Ibalizumab]]<sup>†</sup> ~~\| group5 = Chimerici + umanizzati<br />("-lixizu-")~~ ~~\| list5 = [[Dorlixizumab]] • [[Otelixizumab]]~~ }} ~~\| group2 = [[Interleukina]]<br /> ("-k(i[n])-")~~ ~~\| list2 = {{Navbox subgroup~~ ~~\| group1 = Umani<br /> ("-kinu-")~~ ~~\| list1 = [[Briakinumab]] • [[Canakinumab]] • [[Ustekinumab]]~~ ~~\| group2 = Umanizzati<br /> ("-kizu-")~~ ~~\| list2 = [[Lebrikizumab]]~~ }} ~~\| group11 = Inflammatorie [[lesioni]]<br /> ("-les-")~~ ~~\| list11 = {{Navbox subgroup~~ ~~\| group1 = topo<br /> ("-leso-")~~ ~~\| list1 = [[Besilesomab]] • [[Technetium (99mTc) fanolesomab\|Fanolesomab]]<sup>‡</sup> • [[Lemalesomab]] • [[Technetium (99mTc) sulesomab\|Sulesomab]]~~ }} ~~\| belowstyle = background: transparent; padding: 0px;~~ ~~\| below = {{PharmNavFootnote}}{{Lymph cell navs}}~~ }} ~~{{Navbox~~ ~~\|name = Anticorpi monoclonali per i tumori~~ ~~\|title = [[Anticorpi monoclonali]] per i tumori~~ ~~\|image =~~ ~~\|above =~~ ~~\| group3 = [[Tumore]]<br /> ("-t(u[m])-")~~ ~~\| list3 = {{Navbox subgroup~~ ~~\| group1 = Umano<br /> ("-tumu-")~~ \| list1 = [[Adecatumumab]] • [[Belimumab]] • [[Cixutumumab]] • [[Conatumumab]] • [[Figitumumab]] • [[Glembatumumab vedotin]] • [[Iratumumab]] • [[Lexatumumab]] • [[Lucatumumab]] • [[Mapatumumab]] • [[Necitumumab]] • [[Ofatumumab]] • [[Olaratumab]] • [[Panitumumab]] • [[Pritumumab]] • [[Robatumumab]] • [[Technetium (99mTc) votumumab\|Votumumab]] • [[Zalutumumab]] ~~\| group2 = Topo<br /> ("-tumo-")~~ \| list2 = [[Indium (111In) altumomab pentetate\|Altumomab pentetate]] • [[Anatumomab mafenatox]] • [[Technetium (99mTc) arcitumomab\|Arcitumomab]] • [[Bectumomab]] • [[Blinatumomab]] • [[Iodine (125I) CC49\|CC49]] • [[Detumomab]] • [[Ibritumomab tiuxetan]] • [[Minretumomab]] • [[Mitumomab]] • [[Naptumomab estafenatox]] • [[Technetium (99mTc) nofetumomab merpentan\|Nofetumomab merpentan]] • [[Pemtumomab]] • [[Technetium (99mTc) pintumomab\|Pintumomab]] • [[Indium (111In) satumomab pendetide\|Satumomab pendetide]] • [[Taplitumomab paptox]] • [[Tenatumomab]] • [[Tositumomab]] • [[3F8]] ~~"-govo-" ([[Tumore dell'ovaio]]): [[Abagovomab]] • [[Indium (111In) igovomab\|Igovomab]] • [[Oregovomab]]~~ ~~"-pro-" ([[Carcinoma della prostata\|Tumore prostatico]]): [[Indium (111In) capromab pendetide\|Capromab pendetide]]~~ ~~"-colo-" ([[Tumore del colon]]): [[Edrecolomab]] • [[Nacolomab tafenatox]]~~ ~~\| group3 = [[anticorpo chimerico\|Chimerico]]<br /> ("-tuxi-")~~ ~~\| list3 = [[Bavituximab]] • [[Brentuximab vedotin]] • [[Cetuximab]] • [[Siltuximab]] • [[Rituximab]]<br />~~ ~~"-mexi-" ([[Melanoma]]): [[Ecromeximab]]~~ ~~\| group4 = [[Anticorpo umanizzato\|Umanizzato]]<br /> ("-tuzu-")~~ \| list4 = [[Afutuzumab]] • [[Alemtuzumab]] • [[Bevacizumab]] • [[Bivatuzumab mertansine]] • [[Cantuzumab mertansine]] • [[Citatuzumab bogatox]] • [[Dacetuzumab]] • [[Elotuzumab]]<sup>†</sup> • [[Etaracizumab]] • [[Farletuzumab]] • [[Gemtuzumab ozogamicin]] • [[Inotuzumab ozogamicin]] • [[Labetuzumab]] • [[Lintuzumab]] • [[Matuzumab]]<sup>§</sup> • [[Milatuzumab]] • [[Nimotuzumab]] • [[Oportuzumab monatox]] • [[Pertuzumab]] • [[Sibrotuzumab]] • [[Tacatuzumab tetraxetan]] • [[Tigatuzumab]] • [[Trastuzumab]] • [[Tucotuzumab celmoleukin]] • [[Veltuzumab]] ~~\| group5 = [[Anticorpi trifunctionali\|Ratto/topo ibrido]]<br /> ("-tumaxo-")~~ ~~\| list5 = [[Catumaxomab]] • [[Ertumaxomab]]~~ }} ~~\| below = {{PharmNavFootnote}}~~ }} ~~{{Portale\|medicina}}~~ [[Categoria:Chemioterapici]] [[Categoria:Anticorpi monoclonali]] ~~[[de:Denosumab]]~~ ~~[[en:Denosumab]]~~ ~~[[es:Denosumab]]~~