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tepotinib  (MedChemExpress)


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    MedChemExpress tepotinib
    Tepotinib, supplied by MedChemExpress, used in various techniques. Bioz Stars score: 93/100, based on 5 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
    https://www.bioz.com/result/tepotinib/product/MedChemExpress
    Average 93 stars, based on 5 article reviews
    tepotinib - by Bioz Stars, 2026-02
    93/100 stars

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    Fig. 3. Efficacy of <t>tepotinib</t> in ALK-rearranged NSCLC cell lines. (A) Immunoblot analysis of the indicated proteins in H3122, ABC-19, and ABC-11 cells treated with DMSO, tepotinib, alectinib, or their combination for 24 h. B, MTT assay results for H3122, ABC-19, and ABC-11 cells treated with DMSO, tepotinib, alectinib, or their combination for 72 h. Statistical significance is indicated as follows: ****P < 0.0001, ***P < 0.001, **P < 0.01, *P < 0.05 from cell and DMSO controls. (C) Crystal violet staining of cancer cells after six days of treatment with 1 μmol/L alectinib combined with 2 μmol/L tepotinib. Alec, alectinib; Tep, tepotinib. (For interpretation of the references to colour in this figure legend, the reader is referred to the web version of this article.)
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    Image Search Results


    Arithmetic mean (± standard deviation for linear plot) tepotinib plasma concentration‐time profiles for tepotinib administered alone and in the presence of itraconazole. The horizontal line indicates the lower limit of quantification.

    Journal: Clinical and Translational Science

    Article Title: Sensitivity of Tepotinib to Inhibitors or Inducers of CYP3A4 and P‐Gp: Drug Interaction Studies and Physiologically‐Based Pharmacokinetic Analysis

    doi: 10.1111/cts.70273

    Figure Lengend Snippet: Arithmetic mean (± standard deviation for linear plot) tepotinib plasma concentration‐time profiles for tepotinib administered alone and in the presence of itraconazole. The horizontal line indicates the lower limit of quantification.

    Article Snippet: The systemic clearance of tepotinib (as assessed following IV administration) is 12.8 L/h (~3 mL/min/kg), translating to a blood clearance of approximately 3–5 mL/min/kg, based on a blood: plasma ratio of 0.6–1.0 (the healthcare business of Merck KGaA, Darmstadt, Germany; data on file), indicating a hepatic extraction ratio of approximately 0.15–0.25.

    Techniques: Standard Deviation, Clinical Proteomics, Concentration Assay

    Arithmetic mean (± standard deviation for linear plot) tepotinib plasma concentration‐time profiles for tepotinib administered alone and in the presence of carbamazepine. The horizontal line indicates the lower limit of quantification.

    Journal: Clinical and Translational Science

    Article Title: Sensitivity of Tepotinib to Inhibitors or Inducers of CYP3A4 and P‐Gp: Drug Interaction Studies and Physiologically‐Based Pharmacokinetic Analysis

    doi: 10.1111/cts.70273

    Figure Lengend Snippet: Arithmetic mean (± standard deviation for linear plot) tepotinib plasma concentration‐time profiles for tepotinib administered alone and in the presence of carbamazepine. The horizontal line indicates the lower limit of quantification.

    Article Snippet: The systemic clearance of tepotinib (as assessed following IV administration) is 12.8 L/h (~3 mL/min/kg), translating to a blood clearance of approximately 3–5 mL/min/kg, based on a blood: plasma ratio of 0.6–1.0 (the healthcare business of Merck KGaA, Darmstadt, Germany; data on file), indicating a hepatic extraction ratio of approximately 0.15–0.25.

    Techniques: Standard Deviation, Clinical Proteomics, Concentration Assay

    Tepotinib PBPK modeling. Panels A and B present simulated mean plasma concentration profiles and 90% prediction intervals (solid lines and shading) and mean observed plasma concentrations (dots) from Study 1 (A, N = 17) and Study 2 (B, N = 18), respectively. (Panel C) presents simulated geometric mean ratios (GMR) with 90% CI ( N = 400) for AUC 0‐∞ and C max (itraconazole coadministration) for different f mCYP3A4 , and with and without contribution of hepatic P‐gp to elimination and observed GMR with 90% CI from Study 1 ( N = 17). AUC, area under the curve; CI, confidence interval; C max , maximal plasma concentration; f mCYP3A4 , fraction metabolized by CYP3A4; GMR, geometric mean ratio; PBPK, physiologically‐based pharmacokinetic.

    Journal: Clinical and Translational Science

    Article Title: Sensitivity of Tepotinib to Inhibitors or Inducers of CYP3A4 and P‐Gp: Drug Interaction Studies and Physiologically‐Based Pharmacokinetic Analysis

    doi: 10.1111/cts.70273

    Figure Lengend Snippet: Tepotinib PBPK modeling. Panels A and B present simulated mean plasma concentration profiles and 90% prediction intervals (solid lines and shading) and mean observed plasma concentrations (dots) from Study 1 (A, N = 17) and Study 2 (B, N = 18), respectively. (Panel C) presents simulated geometric mean ratios (GMR) with 90% CI ( N = 400) for AUC 0‐∞ and C max (itraconazole coadministration) for different f mCYP3A4 , and with and without contribution of hepatic P‐gp to elimination and observed GMR with 90% CI from Study 1 ( N = 17). AUC, area under the curve; CI, confidence interval; C max , maximal plasma concentration; f mCYP3A4 , fraction metabolized by CYP3A4; GMR, geometric mean ratio; PBPK, physiologically‐based pharmacokinetic.

    Article Snippet: The systemic clearance of tepotinib (as assessed following IV administration) is 12.8 L/h (~3 mL/min/kg), translating to a blood clearance of approximately 3–5 mL/min/kg, based on a blood: plasma ratio of 0.6–1.0 (the healthcare business of Merck KGaA, Darmstadt, Germany; data on file), indicating a hepatic extraction ratio of approximately 0.15–0.25.

    Techniques: Clinical Proteomics, Concentration Assay

    Drugs submitted to EAMS.

    Journal: JRSM Open

    Article Title: The UK's Early Access to Medicines Scheme 10 years on: an evaluation using publicly available data

    doi: 10.1177/20542704251317916

    Figure Lengend Snippet: Drugs submitted to EAMS.

    Article Snippet: 13 , Tepotinib , Tepmetko , Advanced non-small cell lung cancer , Merck Serono.

    Techniques: Infection, Mutagenesis, Translocation Assay

    Past or ongoing clinical studies of NSCLC with METΔ14ex

    Journal: Journal of Cancer Research and Clinical Oncology

    Article Title: Advances in clinical research of MET exon 14 skipping mutations in non-small cell lung cancer

    doi: 10.1007/s00432-025-06115-y

    Figure Lengend Snippet: Past or ongoing clinical studies of NSCLC with METΔ14ex

    Article Snippet: Tepotinib (Ib) , VISION (Globenewswire ) , NCT02864992 , II , 99 , ORR: 46% mPFS: 8.5 , Peripheral edema nausea.

    Techniques:

    When and by country the medicines are available

    Journal: Journal of Cancer Research and Clinical Oncology

    Article Title: Advances in clinical research of MET exon 14 skipping mutations in non-small cell lung cancer

    doi: 10.1007/s00432-025-06115-y

    Figure Lengend Snippet: When and by country the medicines are available

    Article Snippet: Tepotinib (Ib) , VISION (Globenewswire ) , NCT02864992 , II , 99 , ORR: 46% mPFS: 8.5 , Peripheral edema nausea.

    Techniques:

    Fig. 3. Efficacy of tepotinib in ALK-rearranged NSCLC cell lines. (A) Immunoblot analysis of the indicated proteins in H3122, ABC-19, and ABC-11 cells treated with DMSO, tepotinib, alectinib, or their combination for 24 h. B, MTT assay results for H3122, ABC-19, and ABC-11 cells treated with DMSO, tepotinib, alectinib, or their combination for 72 h. Statistical significance is indicated as follows: ****P < 0.0001, ***P < 0.001, **P < 0.01, *P < 0.05 from cell and DMSO controls. (C) Crystal violet staining of cancer cells after six days of treatment with 1 μmol/L alectinib combined with 2 μmol/L tepotinib. Alec, alectinib; Tep, tepotinib. (For interpretation of the references to colour in this figure legend, the reader is referred to the web version of this article.)

    Journal: Lung cancer (Amsterdam, Netherlands)

    Article Title: Efficacy of amivantamab, a bi-specific antibody targeting EGFR and MET, in ALK-rearranged non-small-cell lung cancer cell lines.

    doi: 10.1016/j.lungcan.2025.108415

    Figure Lengend Snippet: Fig. 3. Efficacy of tepotinib in ALK-rearranged NSCLC cell lines. (A) Immunoblot analysis of the indicated proteins in H3122, ABC-19, and ABC-11 cells treated with DMSO, tepotinib, alectinib, or their combination for 24 h. B, MTT assay results for H3122, ABC-19, and ABC-11 cells treated with DMSO, tepotinib, alectinib, or their combination for 72 h. Statistical significance is indicated as follows: ****P < 0.0001, ***P < 0.001, **P < 0.01, *P < 0.05 from cell and DMSO controls. (C) Crystal violet staining of cancer cells after six days of treatment with 1 μmol/L alectinib combined with 2 μmol/L tepotinib. Alec, alectinib; Tep, tepotinib. (For interpretation of the references to colour in this figure legend, the reader is referred to the web version of this article.)

    Article Snippet: Alectinib [33], erlotinib [34], and tepotinib [35] were purchased from Selleck Chemicals (Houston, TX, USA) and dissolved in dimethyl sulfoxide for in-vitro studies.

    Techniques: Western Blot, MTT Assay, Staining

    Fig. 4. Effects of PBMC co-culture and Fc receptor inhibition on tumor cell response to drug treatments. (A) Crystal violet staining of tumor cells treated for seven days with PBMCs and drugs. Tumor cells were co-cultured with PBMCs at 5 × 106 cells per well and treated with 1 μmol/L alectinib, 2 μmol/L erlotinib, 2 μmol/L tepotinib, or 1000 μg/mL amivantamab. Alec, alectinib; Erl, erlotinib; Tep, tepotinib; Ami, amivantamab. (B) Crystal violet staining to assess the effect of Fc receptor inhibition on amivantamab in the presence of alectinib and PBMCs. Tumor cells were co-cultured for seven days with 5 × 106 PBMCs per well, treated or untreated with an Fc receptor-binding inhibitor polyclonal antibody, 1 μmol/L alectinib, and 1000 μg/mL amivantamab and then stained with crystal violet. (For interpretation of the references to colour in this figure legend, the reader is referred to the web version of this article.)

    Journal: Lung cancer (Amsterdam, Netherlands)

    Article Title: Efficacy of amivantamab, a bi-specific antibody targeting EGFR and MET, in ALK-rearranged non-small-cell lung cancer cell lines.

    doi: 10.1016/j.lungcan.2025.108415

    Figure Lengend Snippet: Fig. 4. Effects of PBMC co-culture and Fc receptor inhibition on tumor cell response to drug treatments. (A) Crystal violet staining of tumor cells treated for seven days with PBMCs and drugs. Tumor cells were co-cultured with PBMCs at 5 × 106 cells per well and treated with 1 μmol/L alectinib, 2 μmol/L erlotinib, 2 μmol/L tepotinib, or 1000 μg/mL amivantamab. Alec, alectinib; Erl, erlotinib; Tep, tepotinib; Ami, amivantamab. (B) Crystal violet staining to assess the effect of Fc receptor inhibition on amivantamab in the presence of alectinib and PBMCs. Tumor cells were co-cultured for seven days with 5 × 106 PBMCs per well, treated or untreated with an Fc receptor-binding inhibitor polyclonal antibody, 1 μmol/L alectinib, and 1000 μg/mL amivantamab and then stained with crystal violet. (For interpretation of the references to colour in this figure legend, the reader is referred to the web version of this article.)

    Article Snippet: Alectinib [33], erlotinib [34], and tepotinib [35] were purchased from Selleck Chemicals (Houston, TX, USA) and dissolved in dimethyl sulfoxide for in-vitro studies.

    Techniques: Co-Culture Assay, Inhibition, Staining, Cell Culture, Binding Assay