A phase I dose escalation study of BIBW 2992, an irreversible dual inhibitor of epidermal growth factor receptor 1 (EGFR) and 2 (HER2) tyrosine kinase in a 2-week on, 2-week off schedule in patients with advanced solid tumours

Eskens, F.; Mom, Constantijne H.; Planting, A. S. T.; Gietema, Jourik A.; Amelsberg, A.; Huisman, Holger; Doorn, Leni van; Burger, Huibert; Stopfer, Peter; Verweij, Jaap; Vries, de Elisabeth G. E.

doi:10.1038/sj.bjc.6604108

Cited by 212 publications

(174 citation statements)

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“…Daily oral treatment with BIBW2992 at 20 mg/kg for 25 days resulted in dramatic tumor regression with a cumulative treated/control tumor volume ratio (T/C ratio) of 2% (Figure 3a), and downregulation of EGFR and AKT phosphorylation, as detected by immunohistochemical staining of tissue sections ( Figure 3b). With this dose schedule, the animals showed no clinical signs of intolerability and gained weight similar to untreated littermates, with systemic exposure (C max , AUC 0À24 h in Supplementary Table 5) comparable to the pharmacokinetic data seen in Phase I studies with effective doses of BIBW2992 (Eskens et al, 2008). When drugs were given at respective maximum tolerated doses in the A431 model, BIBW2992 was more potent than either gefitinib (T/C ¼ 46% at 75 mg/kg/day) or lapatinib (T/C ¼ 32% at 2 Â 100 mg/kg/day) (data not shown).…”

Section: Bibw2992 Inhibits Survival Of Human Nsclc Cell Linesmentioning

confidence: 65%

“…Furthermore, treatment of NIH-3T3 cells expressing the EGFR mutants with BIBW2992 inhibited receptor autophosphorylation at least 100-fold more effectively than erlotinib (Figure 1b). IC 50s for inhibition in these cell-based transformation models are generally well below 300 nM, the maximum achievable drug plasma concentration (Eskens et al, 2008). One notable exception is the A549 cells, which express wild-type EGFR and HER2 and are resistant to BIBW2992.…”

Section: Discussionmentioning

confidence: 99%

“…inhibits EGFR and HER2 kinase activity in vitro BIBW2992, an anilino-quinazoline designed as an irreversible, dual EGFR/HER2 inhibitor, possesses a functional Michael acceptor group similar to the one found in the quinoline-derived irreversible EGFR inhibitors EKB-569 and HKI-272, allowing covalent modification of the ATP-binding site of the kinase domains of EGFR (Cys 773) and HER2 (Cys 805) (Rabindran et al, 2004;Eskens et al, 2008). In cell-free in vitro kinase assays, BIBW2992 shows potent activity against wild-type and mutant forms of EGFR and HER2, similar to gefitinib in potency for L858R EGFR, but about 100-fold more active against the gefitinibresistant L858R-T790M EGFR double mutant, with an IC 50 of 10 nM (Table 1).…”

Section: Bibw2992mentioning

confidence: 99%

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BIBW2992, an irreversible EGFR/HER2 inhibitor highly effective in preclinical lung cancer models

et al. 2008

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Genetic alterations in the kinase domain of the epidermal growth factor receptor (EGFR) in non-small cell lung cancer (NSCLC) patients are associated with sensitivity to treatment with small molecule tyrosine kinase inhibitors. Although first-generation reversible, ATP-competitive inhibitors showed encouraging clinical responses in lung adenocarcinoma tumors harboring such EGFR mutations, almost all patients developed resistance to these inhibitors over time. Such resistance to firstgeneration EGFR inhibitors was frequently linked to an acquired T790M point mutation in the kinase domain of EGFR, or upregulation of signaling pathways downstream of HER3. Overcoming these mechanisms of resistance, as well as primary resistance to reversible EGFR inhibitors driven by a subset of EGFR mutations, will be necessary for development of an effective targeted therapy regimen. Here, we show that BIBW2992, an anilino-quinazoline designed to irreversibly bind EGFR and HER2, potently suppresses the kinase activity of wild-type and activated EGFR and HER2 mutants, including erlotinib-resistant isoforms. Consistent with this activity, BIBW2992 suppresses transformation in isogenic cell-based assays, inhibits survival of cancer cell lines and induces tumor regression in xenograft and transgenic lung cancer models, with superior activity over erlotinib. These findings encourage further testing of BIBW2992 in lung cancer patients harboring EGFR or HER2 oncogenes.

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Section: Bibw2992 Inhibits Survival Of Human Nsclc Cell Linesmentioning

confidence: 65%

Section: Discussionmentioning

confidence: 99%

Section: Bibw2992mentioning

confidence: 99%

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BIBW2992, an irreversible EGFR/HER2 inhibitor highly effective in preclinical lung cancer models

et al. 2008

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“…Дерматологические НЯ, такие как папуло-пустулезная (угревая) сыпь, зуд, сухость/трещины кожи, алопеция, гипертрихоз и паронихия, описывались у онкологических больных, получавших ИТК-EGFR [29]. В клинических иссле-дованиях ИТК-EGFR III фазы у 54-89% пациентов наблю-дались кожные НЯ любой степени и 0-16,2% -НЯ ≥ 3 степени [29][30][31][32][33][34][35][36][37][38][39][40][41]. Критерии NCI-CTCAE являются стандар-том классификации и методом оценки степени тяжести, широко используемым всем онкологическим сообществом при описании НЯ в клинических исследованиях терапии рака.…”

Section: дерматологические нежелательные явленияunclassified

Algorithms for Management of Patients With Adverse Events on Therapy With Tyrosine Kinase Inhibitors Egfr

Сакаева¹

2017

Med. sov.

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С емейство рецепторов ErbB является одной из наиболее широко изученных систем передачи сигналов [1]. Семейство ErbB включает четыре мембранно-связанных структурно родственных рецепто-ра тирозинкиназы: рецептор EGF (EGFR; также известен как ErbB1), HER2 (ErbB2), ErbB3 и ErbB4 [2]. Путь ErbB является одной из наиболее широко изученных систем передачи сигналов, вовлеченных в функционирование нормальных клеток, и при некоторых типах рака [1]. Нарушение регуляции активности рецепторов семейства ErbB и нисходящих сигнальных путей связано с развити-ем некоторых опухолей у человека.Механизм активации передачи сигналов ErbB зависит от лиганд-индуцированной стабильности гомо-или гете-родимеров, образованных различными тирозинкиназами рецепторов семейства ErbB [3]. Рецепторы семейства ErbB являются клинически доказанными мишенями для новых противоопухолевых препаратов [4][5][6][7].Ингибиторы EGFR показаны для лечения колорек-тального рака (панитумумаб, цетуксимаб), немелкокле-точного рака легкого (гефитиниб, эрлотиниб, афатиниб), плоскоклеточного рака головы и шеи (цетуксимаб), рака поджелудочной железы (эрлотиниб).В отличие от цитотоксической химиотерапии, лечение ингибиторами EGFR сопровождается минимальными неспеци фическими и гематологическими побочными эффектами.Активирующие мутации гена рецептора EGFR явля-ются наиболее значимыми предикторами ответа на ингибиторы тирозинкиназы EGFR (ИТК-EGFR) гефити- Ключевые слова: местнораспространенный и метастатический немелкоклеточный рак легкого, ингибиторы тирозин-киназы EGFR, терапия, нежелательные явления. D.D. SAKAEVA, MD, Prof., Republican Oncologic Dispensary of the Ministry of Health of the Republic of Bashkortostan, Ufa ALGORITHMS FOR MANAGEMENT OF PATIENTS WITH ADVERSE EVENTS ON THERAPY WITH TYROSINE KINASE INHIBITORS EGFRThe tyrosine kinase inhibitors (TKIs) of the epidermal receptor growth factor (EGFR) such as gefitinib, erlotinib and afatinib, are the standard first-line therapy in locally advanced and metastatic non-small cell lung cancer (NSCLC) with frequent mutations of the EGFR gene. These drugs are more effective from the point of view of frequency response (FR) and survival without progression (SWP), less toxic and better tolerated than the standard two-component chemotherapy based on platinum drugs. The most frequent adverse events (AE) are gastrointestinal (GI) (diarrhea and stomatitis/mucositis) and dermatological (rash, dry skin and paronychia). They are usually mild, but in some cases symptoms can be moderate and more severity and have a negative impact on quality of life (QOL) of the patient and can require dose adjustment or discontinuation of treatment. Management of AEs, including preventive measures, supportive therapy, temporary cancellation and a reduction in the dose of the drug is important. Recommendations for the prevention and treatment of dermatological toxicity (rash, dry skin and paronychia) and toxicity for the gastrointestinal tract (diarrhoea, stomatitis and mucositis) related to therapy TKI-EGFR are developed. These guidelines descri...

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“…This inhibitor has demonstrated improvements over first-generation EGFR inhibitors in lung cancer and squamous cell carcinoma models [47][48][49]. Tolerability and pharmacokinetics of the inhibitor in patients have recently been investigated in a phase I study by Eskens et al [50], and phase II results reporting clinical activity of the compound have been described [51][52][53].…”

Section: Egf Family Inhibitorsmentioning

confidence: 99%

Radiotherapy and inhibition of the EGF family as treatment strategies for prostate cancer: combining theragnostics with theragates

2010

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A phase I dose escalation study of BIBW 2992, an irreversible dual inhibitor of epidermal growth factor receptor 1 (EGFR) and 2 (HER2) tyrosine kinase in a 2-week on, 2-week off schedule in patients with advanced solid tumours

Cited by 212 publications

References 20 publications

BIBW2992, an irreversible EGFR/HER2 inhibitor highly effective in preclinical lung cancer models

BIBW2992, an irreversible EGFR/HER2 inhibitor highly effective in preclinical lung cancer models

Algorithms for Management of Patients With Adverse Events on Therapy With Tyrosine Kinase Inhibitors Egfr

Radiotherapy and inhibition of the EGF family as treatment strategies for prostate cancer: combining theragnostics with theragates

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