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1. Targeting the EGF receptor family in non-small cell lung cancer—increased complexity and future perspectives

Author

Tobias Boch, Jens Köhler, Melanie Janning, and Sonja Loges

Subjects
oncology, nsclc, egfr, her2, her3, her4, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Lung cancer remains the leading cause of cancer-associated mortality worldwide, but with the emergence of oncogene targeted therapies, treatment options have tremendously improved. Owing to their biological relevance, members of the ERBB receptor family, including the EGF receptor (EGFR), HER2, HER3 and HER4, are among the best studied oncogenic drivers. Activating EGFR mutations are frequently observed in non-small cell lung cancer (NSCLC), and small molecule tyrosine kinase inhibitors (TKIs) are the established first line treatment option for patients whose tumors bear “typical/classical” EGFR mutations (exon 19 deletions, L858R point mutations). Additionally, new TKIs are rapidly evolving with better efficacy to overcome primary and secondary treatment resistance (e.g., that due to T790M or C797S resistance mutations). Some atypical EGFR mutations, such as the most frequent exon 20 insertions, exhibit relative resistance to earlier generation TKIs through steric hindrance. In this subgroup, newer TKIs, such as mobocertinib and the bi-specific antibody amivantamab have recently been approved, whereas less frequent atypical EGFR mutations remain understudied. In contrast to EGFR, HER2 has long remained a challenging target, but better structural understanding has led to the development of newer generations of TKIs. The recent FDA approval of the antibody-drug conjugate trastuzumab-deruxtecan for pretreated patients with HER2 mutant NSCLC has been an important therapeutic breakthrough. HER3 and HER4 also exert oncogenic potential, and targeted treatment approaches are being developed, particularly for HER3. Overall, strategies to inhibit the oncogenic function of ERBB receptors in NSCLC are currently evolving at an unprecedented pace; therefore, this review summarizes current treatment standards and discusses the outlook for future developments.

Published
2022
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2. Unbiased RNA-Seq-driven identification and validation of reference genes for quantitative RT-PCR analyses of pooled cancer exosomes

Author

Yao Dai, Yumeng Cao, Jens Köhler, Aiping Lu, Shaohua Xu, and Haiyun Wang

Subjects
Reference gene, qRT-PCR, Cancer exosome, RNA-Seq, miRNA-Seq, Biotechnology, TP248.13-248.65, Genetics, QH426-470
Abstract

Abstract Background Exosomes are extracellular vesicles (EVs) derived from endocytic compartments of eukaryotic cells which contain various biomolecules like mRNAs or miRNAs. Exosomes influence the biologic behaviour and progression of malignancies and are promising candidates as non-invasive diagnostic biomarkers or as targets for therapeutic interventions. Usually, quantitative real-time polymerase chain reaction (qRT-PCR) is used to assess gene expression in cancer exosomes, however, the ideal reference genes for normalization yet remain to be identified. Results In this study, we performed an unbiased analysis of high-throughput mRNA and miRNA-sequencing data from exosomes of patients with various cancer types and identify candidate reference genes and miRNAs in cancer exosomes. The expression stability of these candidate reference genes was evaluated by the coefficient of variation “CV” and the average expression stability value “M”. We subsequently validated these candidate reference genes in exosomes from an independent cohort of ovarian cancer patients and healthy control individuals by qRT-PCR. Conclusions Our study identifies OAZ1 and hsa-miR-6835-3p as the most reliable individual reference genes for mRNA and miRNA quantification, respectively. For superior accuracy, we recommend the use of a combination of reference genes - OAZ1/SERF2/MPP1 for mRNA and hsa-miR-6835-3p/hsa-miR-4468-3p for miRNA analyses.

Published
2021
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3. Therapeutic Response-Based Reclassification of Multiple Tumor Subtypes Reveals Intrinsic Molecular Concordance of Therapy Across Histologically Disparate Cancers

Author

Yue Xu, Jie Zheng, Zhaoqing Cai, Wang Li, Jens Köhler, Yao Dai, Xiaojie Cheng, Tao Wu, Fan Zhang, and Haiyun Wang

Subjects
tumor classification, OMICS data, pharmacological subtypes, precision medicine, CGP dataset, Biology (General), QH301-705.5
Abstract

Cancers that are histologically defined as the same type of cancer often need a distinct therapy based on underlying heterogeneity; likewise, histologically disparate cancers can require similar treatment approaches due to intrinsic similarities. A comprehensive analysis integrated with drug response data and molecular alterations, particularly to reveal therapeutic concordance mechanisms across histologically disparate tumor subtypes, has not yet been fully exploited. In this study, we integrated pharmacological, genomic, and transcriptomic profiling data provided from the Cancer Genome Project (CGP) in a systematic in silico investigation of the pharmacological subtypes of cancers and the intrinsic concordance of molecular mechanisms leading to similar therapeutic responses across histologically disparate tumor subtypes. We further developed a novel approach to redefine cell-to-cell similarity and drug-to-drug similarity from the therapeutic concordance, providing a new point of view to study cancer heterogeneity. This study demonstrates how pharmacological and omics data can be used to systematically classify cancers in terms of response to various compounds and provides us with a purely therapy-oriented perspective to view tumor classifications independent of histology subtypes. The knowledge of pharmacological subtypes of 367 drugs are available via our website (http://www.hywanglab.cn/dtdb/), providing the resources for precision medicine in the perspective of therapeutic response-based re-classification of tumor.

Published
2021
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4. Synthesis and Antioxidative Properties of 1,2,3,4-Tetrahydropyridine Derivatives with Different Substituents in 4-Position

Author

Daniele Aiello, Hendrik Jonas, Anna Carbone, Daniela Carbone, Camilla Pecoraro, Luisa Tesoriere, Jens Köhler, Bernhard Wünsch, and Patrizia Diana

Subjects
indicaxanthins, betalamic acid, antioxidant, dehydrobromination, TEMPO oxidation, (E)-(Z) configuration, Organic chemistry, QD241-441
Abstract

Natural products are an excellent source of inspiration for the development of new drugs. Among them, betalains have been extensively studied for their antioxidant properties and potential application as natural food dyes. Herein, we describe the seven-step synthesis of new betalamic acid analogs without carboxy groups in the 2- and 6-position with an overall yield of ~70%. The Folin–Ciocalteu assay was used to determine the antioxidant properties of protected intermediate 21. Additionally, the five-step synthesis of betalamic acid analog 35 with three ester moieties was performed. Using NMR techniques, the stability of the obtained compounds towards oxygen was analyzed.

Published
2022
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5. An integrative pharmacogenomics analysis identifies therapeutic targets in KRAS-mutant lung cancerResearch in context

Author

Haiyun Wang, Qi Lv, Yue Xu, Zhaoqing Cai, Jie Zheng, Xiaojie Cheng, Yao Dai, Pasi A. Jänne, Chiara Ambrogio, and Jens Köhler

Subjects
Medicine, Medicine (General), R5-920
Abstract

Background: KRAS mutations are the most frequent oncogenic aberration in lung adenocarcinoma. KRAS mutant isoforms differentially shape tumour biology and influence drug responses. This heterogeneity challenges the development of effective therapies for patients with KRAS-driven non-small cell lung cancer (NSCLC). Methods: We developed an integrative pharmacogenomics analysis to identify potential drug targets to overcome MEK/ERK inhibitor resistance in lung cancer cell lines with KRAS(G12C) mutation (n = 12). We validated our predictive in silico results with in vitro models using gene knockdown, pharmacological target inhibition and reporter assays. Findings: Our computational analysis identifies casein kinase 2A1 (CSNK2A1) as a mediator of MEK/ERK inhibitor resistance in KRAS(G12C) mutant lung cancer cells. CSNK2A1 knockdown reduces cell proliferation, inhibits Wnt/β-catenin signalling and increases the anti-proliferative effect of MEK inhibition selectively in KRAS(G12C) mutant lung cancer cells. The specific CK2-inhibitor silmitasertib phenocopies the CSNK2A1 knockdown effect and sensitizes KRAS(G12C) mutant cells to MEK inhibition. Interpretation: Our study supports the importance of accurate patient stratification and rational drug combinations to gain benefit from MEK inhibition in patients with KRAS mutant NSCLC. We develop a genotype-based strategy that identifies CK2 as a promising co-target in KRAS(G12C) mutant NSCLC by using available pharmacogenomics gene expression datasets. This approach is applicable to other oncogene driven cancers. Fund: This work was supported by grants from the National Natural Science Foundation of China, the National Key Research and Development Program of China, the Lung Cancer Research Foundation and a Mildred-Scheel postdoctoral fellowship from the German Cancer Aid Foundation. Keywords: Pharmacogenomic profiles, KRAS mutations, Lung adenocarcinoma, CSNK2A1, CK2, MEK inhibitor, Silmitasertib, Wnt/β-catenin, EMT

Published
2019
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6. Cellular responses to beating hydrogels to investigate mechanotransduction

Author

Yashoda Chandorkar, Arturo Castro Nava, Sjören Schweizerhof, Marcel Van Dongen, Tamás Haraszti, Jens Köhler, Hang Zhang, Reinhard Windoffer, Ahmed Mourran, Martin Möller, and Laura De Laporte

Subjects
Science
Abstract

Mechanotransduction of cells is of interest for a number of reasons but model in vitro systems remain a challenge. Here, the authors report on a hydrogel which changes properties upon near infrared irradiation to create cyclic forces and demonstrate the application of these gels to study mechanotransduction.

Published
2019
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7. If Virchow and Ehrlich Had Dreamt Together: What the Future Holds for KRAS-Mutant Lung Cancer

Author

Jens Köhler and Pasi A. Jänne

Subjects
KRAS, lung cancer, NSCLC, G12C inhibitor, immunotherapy, ICI, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Non-small-cell lung cancer (NSCLC) with Kirsten rat sarcoma (KRAS) mutations has notoriously challenged oncologists and researchers for three notable reasons: (1) the historical assumption that KRAS is “undruggable”, (2) the disease heterogeneity and (3) the shaping of the tumor microenvironment by KRAS downstream effector functions. Better insights into KRAS structural biochemistry allowed researchers to develop direct KRAS(G12C) inhibitors, which have shown early signs of clinical activity in NSCLC patients and have recently led to an FDA breakthrough designation for AMG-510. Following the approval of immune checkpoint inhibitors for PDL1-positive NSCLC, this could fuel yet another major paradigm shift in the treatment of advanced lung cancer. Here, we review advances in our understanding of the biology of direct KRAS inhibition and project future opportunities and challenges of dual KRAS and immune checkpoint inhibition. This strategy is supported by preclinical models which show that KRAS(G12C) inhibitors can turn some immunologically “cold” tumors into “hot” ones and therefore could benefit patients whose tumors harbor subtype-defining STK11/LKB1 co-mutations. Forty years after the discovery of KRAS as a transforming oncogene, we are on the verge of approval of the first KRAS-targeted drug combinations, thus therapeutically unifying Paul Ehrlich’s century-old “magic bullet” vision with Rudolf Virchow’s cancer inflammation theory.

Published
2021
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8. Correlation of the apparent diffusion coefficient (ADC) with the standardized uptake value (SUV) in lymph node metastases of non-small cell lung cancer (NSCLC) patients using hybrid 18F-FDG PET/MRI.

Author

Benedikt Michael Schaarschmidt, Christian Buchbender, Felix Nensa, Johannes Grueneisen, Benedikt Gomez, Jens Köhler, Henning Reis, Verena Ruhlmann, Lale Umutlu, and Philipp Heusch

Subjects
Medicine, Science
Abstract

OBJECTIVE:To compare the apparent diffusion coefficient (ADC) in lymph node metastases of non-small cell lung cancer (NSCLC) patients with standardized uptake values (SUV) derived from combined 18F-fluoro-deoxy-glucose-positron emission tomography/magnetic resonance imaging (18F-FDG PET/MRI). MATERIAL AND METHODS:38 patients with histopathologically proven NSCLC (mean age 60.1 ± 9.5 y) received whole-body PET/CT (Siemens mCT™) 60 min after injection of a mean dose of 280 ± 50 MBq 18F-FDG and subsequent PET/MRI (mean time after tracer injection: 139 ± 26 min, Siemens Biograph mMR). During PET acquisition, simultaneous diffusion-weighted imaging (DWI, b values: 0, 500, 1000 s/mm²) was performed. A maximum of 10 lymph nodes per patient suspicious for malignancy were analyzed. Regions of interest (ROI) were drawn covering the entire lymph node on the attenuation-corrected PET-image and the monoexponential ADC-map. According to histopathology or radiological follow-up, lymph nodes were classified as benign or malignant. Pearson's correlation coefficients were calculated for all lymph node metastases correlating SUVmax and SUVmean with ADCmean. RESULTS:A total of 146 suspicious lymph nodes were found in 25 patients. One hundred lymph nodes were eligible for final analysis. Ninety-one lymph nodes were classified as malignant and 9 as benign according to the reference standard. In malignant lesions, mean SUVmax was 9.1 ± 3.8 and mean SUVmean was 6.0 ± 2.5 while mean ADCmean was 877.0 ± 128.6 x10(-5) mm²/s in PET/MRI. For all malignant lymph nodes, a weak, inverse correlation between SUVmax and ADCmean as well as SUVmean and ADCmean (r = -0.30, p

Published
2015
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9. Development of a highly sensitive and specific method for detection of circulating tumor cells harboring somatic mutations in non-small-cell lung cancer patients.

Author

Frank Breitenbuecher, Sandra Hoffarth, Karl Worm, Diana Cortes-Incio, Thomas C Gauler, Jens Köhler, Thomas Herold, Kurt Werner Schmid, Lutz Freitag, Stefan Kasper, and Martin Schuler

Subjects
Medicine, Science
Abstract

BACKGROUND: Oncogenic mutations are powerful predictive biomarkers for molecularly targeted cancer therapies. For mutation detection patients have to undergo invasive tumor biopsies. Alternatively, archival samples are used which may no longer reflect the actual tumor status. Circulating tumor cells (CTC) could serve as an alternative platform to detect somatic mutations in cancer patients. We sought to develop a sensitive and specific assay to detect mutations in the EGFR gene in CTC from lung cancer patients. METHODS: We developed a novel assay based on real-time polymerase chain reaction (PCR) and melting curve analysis to detect activating EGFR mutations in blood cell fractions enriched in CTC. Non-small-cell lung cancer (NSCLC) was chosen as disease model with reportedly very low CTC counts. The assay was prospectively validated in samples from patients with EGFR-mutant and EGFR-wild type NSCLC treated within a randomized clinical trial. Sequential analyses were conducted to monitor CTC signals during therapy and correlate mutation detection in CTC with treatment outcome. RESULTS: Assay sensitivity was optimized to enable detection of a single EGFR-mutant CTC/mL peripheral blood. CTC were detected in pretreatment blood samples from all 8 EGFR-mutant lung cancer patients studied. Loss of EGFR-mutant CTC signals correlated with treatment response, and its reoccurrence preceded relapse. CONCLUSIONS: Despite low abundance of CTC in NSCLC oncogenic mutations can be reproducibly detected by applying an unbiased CTC enrichment strategy and highly sensitive PCR and melting curve analysis. This strategy may enable non-invasive, specific biomarker diagnostics and monitoring in patients undergoing targeted cancer therapies.

Published
2014
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10. Lestaurtinib inhibits histone phosphorylation and androgen-dependent gene expression in prostate cancer cells.

Author

Jens Köhler, German Erlenkamp, Adrien Eberlin, Tobias Rumpf, Inna Slynko, Eric Metzger, Roland Schüle, Wolfgang Sippl, and Manfred Jung

Subjects
Medicine, Science
Abstract

BACKGROUND: Epigenetics is defined as heritable changes in gene expression that are not based on changes in the DNA sequence. Posttranslational modification of histone proteins is a major mechanism of epigenetic regulation. The kinase PRK1 (protein kinase C related kinase 1, also known as PKN1) phosphorylates histone H3 at threonine 11 and is involved in the regulation of androgen receptor signalling. Thus, it has been identified as a novel drug target but little is known about PRK1 inhibitors and consequences of its inhibition. METHODOLOGY/PRINCIPAL FINDING: Using a focused library screening approach, we identified the clinical candidate lestaurtinib (also known as CEP-701) as a new inhibitor of PRK1. Based on a generated 3D model of the PRK1 kinase using the homolog PKC-theta (protein kinase c theta) protein as a template, the key interaction of lestaurtinib with PRK1 was analyzed by means of molecular docking studies. Furthermore, the effects on histone H3 threonine phosphorylation and androgen-dependent gene expression was evaluated in prostate cancer cells. CONCLUSIONS/SIGNIFICANCE: Lestaurtinib inhibits PRK1 very potently in vitro and in vivo. Applied to cell culture it inhibits histone H3 threonine phosphorylation and androgen-dependent gene expression, a feature that has not been known yet. Thus our findings have implication both for understanding of the clinical activity of lestaurtinib as well as for future PRK1 inhibitors.

Published
2012
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12. Supplementary Materials and Methods from Combination of Type I and Type II MET Tyrosine Kinase Inhibitors as Therapeutic Approach to Prevent Resistance

Author

Pasi A. Jänne, Stephen Wang, Sujuan Guo, Jiannan Guo, Paul T. Kirschmeier, Jens Köhler, Zihan Wei, Fangxin Hong, Pratik R. Chopade, Prafulla C. Gokhale, Christie J. Lau, Kshiti H. Dholakia, Nam Doo Kim, Taebo Sim, Luke J. Taus, Yanan Kuang, Cloud P. Paweletz, and Magda Bahcall

Abstract

Application of Bliss independence to test for synergy effect of TKI combination treatment in vivo

Published
2023

13. Data from Combination of Type I and Type II MET Tyrosine Kinase Inhibitors as Therapeutic Approach to Prevent Resistance

Author

Pasi A. Jänne, Stephen Wang, Sujuan Guo, Jiannan Guo, Paul T. Kirschmeier, Jens Köhler, Zihan Wei, Fangxin Hong, Pratik R. Chopade, Prafulla C. Gokhale, Christie J. Lau, Kshiti H. Dholakia, Nam Doo Kim, Taebo Sim, Luke J. Taus, Yanan Kuang, Cloud P. Paweletz, and Magda Bahcall

Abstract

MET-targeted therapies are clinically effective in MET-amplified and MET exon 14 deletion mutant (METex14) non–small cell lung cancers (NSCLCs), but their efficacy is limited by the development of drug resistance. Structurally distinct MET tyrosine kinase inhibitors (TKIs) (type I/II) have been developed or are under clinical evaluation, which may overcome MET-mediated drug resistance mechanisms. In this study, we assess secondary MET mutations likely to emerge in response to treatment with single-agent or combinations of type I/type II MET TKIs using TPR-MET transformed Ba/F3 cell mutagenesis assays. We found that these inhibitors gave rise to distinct secondary MET mutant profiles. However, a combination of type I/II TKI inhibitors (capmatinib and merestinib) yielded no resistant clones in vitro. The combination of capmatinib/merestinib was evaluated in vivo and led to a significant reduction in tumor outgrowth compared with either MET inhibitor alone. Our findings demonstrate in vitro and in vivo that a simultaneous treatment with a type I and type II MET TKI may be a clinically viable approach to delay and/or diminish the emergence of on target MET-mediated drug-resistance mutations.

Published
2023

14. Supplementary Data from Combination of Type I and Type II MET Tyrosine Kinase Inhibitors as Therapeutic Approach to Prevent Resistance

Author

Pasi A. Jänne, Stephen Wang, Sujuan Guo, Jiannan Guo, Paul T. Kirschmeier, Jens Köhler, Zihan Wei, Fangxin Hong, Pratik R. Chopade, Prafulla C. Gokhale, Christie J. Lau, Kshiti H. Dholakia, Nam Doo Kim, Taebo Sim, Luke J. Taus, Yanan Kuang, Cloud P. Paweletz, and Magda Bahcall

Abstract

Supplementary Figures S1-3; Supplementary Tables S1-3

Published
2023

15. Supplementary Data from Comparative Analysis and Isoform-Specific Therapeutic Vulnerabilities of KRAS Mutations in Non–Small Cell Lung Cancer

Author

Chiara Ambrogio, Pasi A. Jänne, Mark M. Awad, Prafulla C. Gokhale, David Santamaria, Marie-Julie Nokin, Elodie Richard, Yunhan Chen, Kshiti H. Dholakia, Jens Köhler, Amanda J. Redig, Chhayheng Chhoeu, Joao Victor Alessi, Yue Xu, Jiaqi Li, Heidi M. Haikala, Mika Lin, Haiyun Wang, Raymond Paranal, Xinan Wang, Yoonji Eum, Enrico Patrucco, Alessia Mira, Jeffrey J. Okoro, Jieun Son, and Biagio Ricciuti

Abstract

Supplementary Data from Comparative Analysis and Isoform-Specific Therapeutic Vulnerabilities of KRAS Mutations in Non–Small Cell Lung Cancer

Published
2023

16. Supplementary Table 2 from EGFR Inhibition Enhances the Cellular Uptake and Antitumor-Activity of the HER3 Antibody–Drug Conjugate HER3–DXd

Author

Pasi A. Jänne, Prafulla C. Gokhale, Cloud P. Paweletz, Yang Qiu, Yasuki Kamai, Yoshinobu Shiose, Channing Yu, Paul T. Kirschmeier, Mari Kuraguchi, Luke J. Taus, Anika E. Adeni, Emily S. Chambers, Brittaney A. Leeper, Arrien A. Bertram, Elena V. Ivanova, Yutong Zhao, Kenneth Ngo, Tyler J. Teceno, Qing Zeng, Man Xu, Pinar O. Eser, Jens Köhler, Timothy Lopez, and Heidi M. Haikala

Abstract

Summary of EGFR inhibitor resistant patient-derived xenografts.

Published
2023

17. Supplementary Table 1 from EGFR Inhibition Enhances the Cellular Uptake and Antitumor-Activity of the HER3 Antibody–Drug Conjugate HER3–DXd

Author

Pasi A. Jänne, Prafulla C. Gokhale, Cloud P. Paweletz, Yang Qiu, Yasuki Kamai, Yoshinobu Shiose, Channing Yu, Paul T. Kirschmeier, Mari Kuraguchi, Luke J. Taus, Anika E. Adeni, Emily S. Chambers, Brittaney A. Leeper, Arrien A. Bertram, Elena V. Ivanova, Yutong Zhao, Kenneth Ngo, Tyler J. Teceno, Qing Zeng, Man Xu, Pinar O. Eser, Jens Köhler, Timothy Lopez, and Heidi M. Haikala

Abstract

Antibodies used in the study

Published
2023

18. Data from EGFR Inhibition Enhances the Cellular Uptake and Antitumor-Activity of the HER3 Antibody–Drug Conjugate HER3–DXd

Author

Pasi A. Jänne, Prafulla C. Gokhale, Cloud P. Paweletz, Yang Qiu, Yasuki Kamai, Yoshinobu Shiose, Channing Yu, Paul T. Kirschmeier, Mari Kuraguchi, Luke J. Taus, Anika E. Adeni, Emily S. Chambers, Brittaney A. Leeper, Arrien A. Bertram, Elena V. Ivanova, Yutong Zhao, Kenneth Ngo, Tyler J. Teceno, Qing Zeng, Man Xu, Pinar O. Eser, Jens Köhler, Timothy Lopez, and Heidi M. Haikala

Abstract

Epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKI) are the standard-of-care treatment for EGFR-mutant non–small cell lung cancers (NSCLC). However, most patients develop acquired drug resistance to EGFR TKIs. HER3 is a unique pseudokinase member of the ERBB family that functions by dimerizing with other ERBB family members (EGFR and HER2) and is frequently overexpressed in EGFR-mutant NSCLC. Although EGFR TKI resistance mechanisms do not lead to alterations in HER3, we hypothesized that targeting HER3 might improve efficacy of EGFR TKI. HER3–DXd is an antibody–drug conjugate (ADC) comprised of HER3-targeting antibody linked to a topoisomerase I inhibitor currently in clinical development. In this study, we evaluated the efficacy of HER3–DXd across a series of EGFR inhibitor–resistant, patient-derived xenografts and observed it to be broadly effective in HER3-expressing cancers. We further developed a preclinical strategy to enhance the efficacy of HER3–DXd through osimertinib pretreatment, which increased membrane expression of HER3 and led to enhanced internalization and efficacy of HER3–DXd. The combination of osimertinib and HER3–DXd may be an effective treatment approach and should be evaluated in future clinical trials in EGFR-mutant NSCLC patients.Significance:EGFR inhibition leads to increased HER3 membrane expression and promotes HER3–DXd ADC internalization and efficacy, supporting the clinical development of the EGFR inhibitor/HER3–DXd combination in EGFR-mutant lung cancer.See related commentary by Lim et al., p. 18

Published
2023

19. Supplementary Table 3 from EGFR Inhibition Enhances the Cellular Uptake and Antitumor-Activity of the HER3 Antibody–Drug Conjugate HER3–DXd

Author

Pasi A. Jänne, Prafulla C. Gokhale, Cloud P. Paweletz, Yang Qiu, Yasuki Kamai, Yoshinobu Shiose, Channing Yu, Paul T. Kirschmeier, Mari Kuraguchi, Luke J. Taus, Anika E. Adeni, Emily S. Chambers, Brittaney A. Leeper, Arrien A. Bertram, Elena V. Ivanova, Yutong Zhao, Kenneth Ngo, Tyler J. Teceno, Qing Zeng, Man Xu, Pinar O. Eser, Jens Köhler, Timothy Lopez, and Heidi M. Haikala

Abstract

Allelic Frequencies in PC-9 vs PC-9 T790M/C797S cells.

Published
2023

20. Data from Comparative Analysis and Isoform-Specific Therapeutic Vulnerabilities of KRAS Mutations in Non–Small Cell Lung Cancer

Author

Chiara Ambrogio, Pasi A. Jänne, Mark M. Awad, Prafulla C. Gokhale, David Santamaria, Marie-Julie Nokin, Elodie Richard, Yunhan Chen, Kshiti H. Dholakia, Jens Köhler, Amanda J. Redig, Chhayheng Chhoeu, Joao Victor Alessi, Yue Xu, Jiaqi Li, Heidi M. Haikala, Mika Lin, Haiyun Wang, Raymond Paranal, Xinan Wang, Yoonji Eum, Enrico Patrucco, Alessia Mira, Jeffrey J. Okoro, Jieun Son, and Biagio Ricciuti

Abstract

Purpose:Activating missense mutations of KRAS are the most frequent oncogenic driver events in lung adenocarcinoma (LUAD). However, KRAS isoforms are highly heterogeneous, and data on the potential isoform-dependent therapeutic vulnerabilities are still lacking.Experimental Design:We developed an isogenic cell-based platform to compare the oncogenic properties and specific therapeutic actionability of KRAS-mutant isoforms. In parallel, we analyzed clinicopathologic and genomic data from 3,560 patients with non–small cell lung cancer (NSCLC) to survey allele-specific features associated with oncogenic KRAS mutations.Results:In isogenic cell lines expressing different mutant KRAS isoforms, we identified isoform-specific biochemical, biological, and oncogenic properties both in vitro and in vivo. These exclusive features correlated with different therapeutic responses to MEK inhibitors, with KRAS G12C and Q61H mutants being more sensitive compared with other isoforms. In vivo, combined KRAS G12C and MEK inhibition was more effective than either drug alone. Among patients with NSCLCs that underwent comprehensive tumor genomic profiling, STK11 and ATM mutations were significantly enriched among tumors harboring KRAS G12C, G12A, and G12V mutations. KEAP1 mutation was significantly enriched among KRAS G12C and KRAS G13X LUADs. KRAS G13X-mutated tumors had the highest frequency of concurrent STK11 and KEAP1 mutations. Transcriptomic profiling revealed unique patterns of gene expression in each KRAS isoform, compared with KRAS wild-type tumors.Conclusions:This study demonstrates that KRAS isoforms are highly heterogeneous in terms of concurrent genomic alterations and gene-expression profiles, and that stratification based on KRAS alleles should be considered in the design of future clinical trials.

Published
2023

21. Supplementary Data from EGFR Inhibition Enhances the Cellular Uptake and Antitumor-Activity of the HER3 Antibody–Drug Conjugate HER3–DXd

Author

Pasi A. Jänne, Prafulla C. Gokhale, Cloud P. Paweletz, Yang Qiu, Yasuki Kamai, Yoshinobu Shiose, Channing Yu, Paul T. Kirschmeier, Mari Kuraguchi, Luke J. Taus, Anika E. Adeni, Emily S. Chambers, Brittaney A. Leeper, Arrien A. Bertram, Elena V. Ivanova, Yutong Zhao, Kenneth Ngo, Tyler J. Teceno, Qing Zeng, Man Xu, Pinar O. Eser, Jens Köhler, Timothy Lopez, and Heidi M. Haikala

Abstract

Supplementary Figures and legends

Published
2023

23. Combination of Type I and Type II MET Tyrosine Kinase Inhibitors as Therapeutic Approach to Prevent Resistance

Author

Magda Bahcall, Luke J. Taus, Taebo Sim, Prafulla C. Gokhale, Jens Köhler, Stephen Wang, Nam Doo Kim, Cloud P. Paweletz, Zihan Wei, Yanan Kuang, Christie J. Lau, Pasi A. Jänne, Pratik R Chopade, Kshiti Dholakia, Sujuan Guo, Fangxin Hong, Jiannan Guo, and Paul Kirschmeier

Subjects
Cancer Research, business.industry, Cell, Mutant, High-Throughput Nucleotide Sequencing, Merestinib, Mutagenesis (molecular biology technique), Drug resistance, Article, In vitro, respiratory tract diseases, Molecular Docking Simulation, Mice, medicine.anatomical_structure, Oncology, Drug Resistance, Neoplasm, In vivo, medicine, Cancer research, Animals, Humans, Female, business, Protein Kinase Inhibitors, Tyrosine kinase
Abstract

MET-targeted therapies are clinically effective in MET-amplified and MET exon 14 deletion mutant (METex14) non–small cell lung cancers (NSCLCs), but their efficacy is limited by the development of drug resistance. Structurally distinct MET tyrosine kinase inhibitors (TKIs) (type I/II) have been developed or are under clinical evaluation, which may overcome MET-mediated drug resistance mechanisms. In this study, we assess secondary MET mutations likely to emerge in response to treatment with single-agent or combinations of type I/type II MET TKIs using TPR-MET transformed Ba/F3 cell mutagenesis assays. We found that these inhibitors gave rise to distinct secondary MET mutant profiles. However, a combination of type I/II TKI inhibitors (capmatinib and merestinib) yielded no resistant clones in vitro. The combination of capmatinib/merestinib was evaluated in vivo and led to a significant reduction in tumor outgrowth compared with either MET inhibitor alone. Our findings demonstrate in vitro and in vivo that a simultaneous treatment with a type I and type II MET TKI may be a clinically viable approach to delay and/or diminish the emergence of on target MET-mediated drug-resistance mutations.

Published
2022

24. EGFR Inhibition Enhances the Cellular Uptake and Antitumor-Activity of the HER3 Antibody–Drug Conjugate HER3–DXd

Author

Man Xu, Tyler Teceno, Pasi A. Jänne, Anika E. Adeni, Paul Kirschmeier, Timothy Lopez, Jens Köhler, Emily S. Chambers, Brittaney A Leeper, Mari Kuraguchi, Elena Ivanova, Arrien A. Bertram, Cloud P. Paweletz, Yoshinobu Shiose, Yutong Zhao, C. Yu, Yasuki Kamai, Luke J. Taus, Kenneth H. Ngo, Qing Zeng, Prafulla C. Gokhale, Heidi M. Haikala, Yang Qiu, and Pinar O. Eser

Subjects
Cancer Research, Antibody-drug conjugate, Immunoconjugates, Receptor, ErbB-3, media_common.quotation_subject, Cell, Cell Culture Techniques, Antineoplastic Agents, Apoptosis, Drug resistance, Mice, Cell Line, Tumor, medicine, Animals, Humans, Osimertinib, Epidermal growth factor receptor, skin and connective tissue diseases, Internalization, media_common, biology, business.industry, respiratory tract diseases, ErbB Receptors, body regions, medicine.anatomical_structure, Oncology, Cancer research, biology.protein, Antibody, business, Tyrosine kinase
Abstract

Epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKI) are the standard-of-care treatment for EGFR-mutant non–small cell lung cancers (NSCLC). However, most patients develop acquired drug resistance to EGFR TKIs. HER3 is a unique pseudokinase member of the ERBB family that functions by dimerizing with other ERBB family members (EGFR and HER2) and is frequently overexpressed in EGFR-mutant NSCLC. Although EGFR TKI resistance mechanisms do not lead to alterations in HER3, we hypothesized that targeting HER3 might improve efficacy of EGFR TKI. HER3–DXd is an antibody–drug conjugate (ADC) comprised of HER3-targeting antibody linked to a topoisomerase I inhibitor currently in clinical development. In this study, we evaluated the efficacy of HER3–DXd across a series of EGFR inhibitor–resistant, patient-derived xenografts and observed it to be broadly effective in HER3-expressing cancers. We further developed a preclinical strategy to enhance the efficacy of HER3–DXd through osimertinib pretreatment, which increased membrane expression of HER3 and led to enhanced internalization and efficacy of HER3–DXd. The combination of osimertinib and HER3–DXd may be an effective treatment approach and should be evaluated in future clinical trials in EGFR-mutant NSCLC patients. Significance: EGFR inhibition leads to increased HER3 membrane expression and promotes HER3–DXd ADC internalization and efficacy, supporting the clinical development of the EGFR inhibitor/HER3–DXd combination in EGFR-mutant lung cancer. See related commentary by Lim et al., p. 18

Published
2022

33. Insights into Ergochromes of the Plant Pathogen Claviceps purpurea

Author

Lena Müller, Christina Stroh, Constantin G. Daniliuc, Jens Köhler, Melanie Esselen, Hans-Ulrich Humpf, Friederike Lünne, Svetlana A. Kalinina, Ernst-Ulrich Würthwein, and Christian Mück-Lichtenfeld

Subjects
Pharmacology, Ergotism, biology, Chemistry, Topoisomerase, Organic Chemistry, Absolute configuration, Pharmaceutical Science, medicine.disease, Claviceps purpurea, biology.organism_classification, Analytical Chemistry, Pigment, chemistry.chemical_compound, Complementary and alternative medicine, Biochemistry, visual_art, Drug Discovery, Xanthone, biology.protein, medicine, visual_art.visual_art_medium, Molecular Medicine, Secalonic acid, Pathogen
Abstract

Claviceps purpurea is an ergot fungus known for its neurotropic alkaloids, which have been identified as the main cause of ergotism, a livestock and human disease triggered by ergot consumption. Tetrahydroxanthone dimers, the so-called ergopigments, presumably also contribute to this toxic effect. Overexpression of the cluster-specific transcription factor responsible for the formation of these pigments in C. purpurea led to the isolation of three new metabolites (8-10). The new pigments were characterized utilizing HRMS, NMR techniques, and CD spectroscopy and shown to be xanthone dimers. Secalonic acid A and its 2,4'- and 4,4'-linked isomers were also isolated, and their absolute configuration was investigated. The contribution of secalonic acid A, its isomers, and new metabolites to the toxicity of C. purpurea was investigated in HepG2 and CCF-STTG1 cells. Along with cytotoxic properties, secalonic acid A was found to inhibit topoisomerase I and II activity.

Published
2021

34. Late-Stage Modification of Aminoglycoside Antibiotics Overcomes Bacterial Resistance Mediated by APH(3') Kinases

Author

Andreas A. Bastian, Maria Bastian, Manuel Jäger, Mark Loznik, Eliza M. Warszawik, Xintong Yang, Nabil Tahiri, Peter Fodran, Martin D. Witte, Anne Thoma, Jens Köhler, Adriaan J. Minnaard, Andreas Herrmann, Stratingh Institute of Chemistry, Chemical Biology 2, and Nanotechnology and Biophysics in Medicine (NANOBIOMED)

Subjects
Aminoglycosides, ddc:540, Organic Chemistry, Drug Resistance, Bacterial, Gram-Negative Bacteria, Phosphotransferases, Humans, General Chemistry, Gram-Positive Bacteria, Catalysis, Anti-Bacterial Agents
Abstract

Chemistry - a European journal 28(36), e202200883 (2022). doi:10.1002/chem.202200883, Published by Wiley-VCH, Weinheim

Published
2022

35. Synthesis and pharmacological evaluation of enantiomerically pure endo-configured KOR agonists with 2-azabicyclo[3.2.1]octane scaffold

Author

Kirstin Lehmkuhl, Patrizia Diana, Hendrik Jonas, Jens Köhler, Dirk Schepmann, Daniele Aiello, Bernhard Wünsch, Bastian Frehland, Hendrik Jona, Daniele Aiello, Bastian Frehland, Kirstin Lehmkuhl, Dirk Schepmann, Jens Köhler, Patrizia Diana, and Bernhard Wünsch

Subjects
chemistry.chemical_classification, Ketone, Bicyclic molecule, Stereochemistry, Organic Chemistry, KOR agonist, opioid receptor, Biochemistry, Reductive amination, Pyrrolidine, Chiral column chromatography, chemistry.chemical_compound, chemistry, Chiral pool synthesis, 2-azabicyclo[3.2.1]octane, Moiety, Physical and Theoretical Chemistry, Enantiomer
Abstract

Conformationally restricted bicyclic KOR agonists 10 with an endo configured amino moiety were synthesized to analyze the bioactive conformation of conformationally flexible KOR agonists such as 2-5. A seven-step, chiral pool synthesis starting with (S)-configured 4-oxopiperidine-2-carboxylate 13 was developed. cis and trans configured diesters 12 were obtained in a 3:1 ratio via hydrogenation of the α,β unsaturated ester 14. After establishment of the bicyclic scaffold, a diastereoselective reductive amination of ketone 11 provided exclusively the endo configured bicyclic amines 10a,b. The 3:1 mixtures of enantiomers were separated by chiral HPLC, respectively, leading to enantiomerically pure KOR agonists (1S,5S,7R)-10a,b and (1R,5R,7S)-10a,b (ent 10a,b). The KOR affinity was determined in receptor binding studies with the radioligand [3H]U-69,593. The high KOR affinity of endo-configured amines 10a (Ki = 7 nM) and 10b (Ki = 13 nM) indicates that the dihedral angle of the KOR pharmacophoric element N(pyrrolidine)-C-C-N(phenylacetyl) of 42° is close to the bioactive conformation of more flexible KOR agonists. It should be noted that changing the configuration of potent and selective KOR agonists 10a and 10b led to potent and selective 1 ligands (e.g. ent-10a Ki(1) = 10 nM).

Published
2021

36. Einmal im Kreis gelaufen - oder der Weg ist das Ziel

Author

Jens Köhler

Abstract

Die Kolumne „Ehrlich und Priesberg“ möchte mit unterhaltsamen Dialogen rund um das Thema „Mensch – Kommunikation, Verhalten, Entscheidungen“ Denkanstöße für den PM-Alltag geben.

Published
2023

37. ERK Inhibitor LY3214996-Based Treatment Strategies forRAS-Driven Lung Cancer

Author

Margaret K. Wilkens, Monica Musteanu, Aine Knott, Magda Bahcall, Shripad V. Bhagwat, Kara M. Soroko, Prafulla C. Gokhale, Jens Köhler, Emily S. Chambers, Mika Lin, Yutong Zhao, Hong L. Tiv, Jihyun Choi, Jason Manro, Ramon V. Tiu, Arrien A. Bertram, Pasi A. Jänne, Atsuko Ogino, Cloud P. Paweletz, Jiaqi Li, and Chiara Ambrogio

Subjects
0301 basic medicine, MAPK/ERK pathway, Cancer Research, business.industry, Gene mutation, medicine.disease, Clinical trial, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Oncology, chemistry, 030220 oncology & carcinogenesis, Toxicity, medicine, Cancer research, Lung cancer, business, Abemaciclib, Function (biology), PI3K/AKT/mTOR pathway
Abstract

RAS gene mutations are the most frequent oncogenic event in lung cancer. They activate multiple RAS-centric signaling networks among them the MAPK, PI3K, and RB pathways. Within the MAPK pathway, ERK1/2 proteins exert a bottleneck function for transmitting mitogenic signals and activating cytoplasmic and nuclear targets. In view of disappointing antitumor activity and toxicity of continuously applied MEK inhibitors in patients with KRAS-mutant lung cancer, research has recently focused on ERK1/2 proteins as therapeutic targets and on ERK inhibitors for their ability to prevent bypass and feedback pathway activation. Here, we show that intermittent application of the novel and selective ATP-competitive ERK1/2 inhibitor LY3214996 exerts single-agent activity in patient-derived xenograft (PDX) models of RAS-mutant lung cancer. Combination treatments were well tolerated and resulted in synergistic (ERKi plus PI3K/mTORi LY3023414) and additive (ERKi plus CDK4/6i abemaciclib) tumor growth inhibition in PDX models. Future clinical trials are required to investigate if intermittent ERK inhibitor-based treatment schedules can overcome toxicities observed with continuous MEK inhibition and—equally important—to identify biomarkers for patient stratification.

Published
2021

40. Physical gels of poly(vinylamine) by thermal curing

Author

Smriti Singh, Martin Möller, Thorsten Fischer, and Jens Köhler

Subjects
Materials science, General Chemical Engineering, technology, industry, and agriculture, Thermal curing, 02 engineering and technology, General Chemistry, 010402 general chemistry, 021001 nanoscience & nanotechnology, Electrochemistry, 01 natural sciences, 0104 chemical sciences, chemistry.chemical_compound, Differential scanning calorimetry, chemistry, Rheology, Dynamic light scattering, Chemical engineering, ddc:540, 0210 nano-technology, Spectroscopy, Ethylene glycol
Abstract

RSC Advances 10(37), 21933-21939 (2020). doi:10.1039/D0RA01607A, Published by RSC Publishing, London

Published
2020

41. Comparative Analysis and Isoform-Specific Therapeutic Vulnerabilities of KRAS Mutations in Non-Small Cell Lung Cancer

Author

Biagio Ricciuti, Jieun Son, Jeffrey J. Okoro, Alessia Mira, Enrico Patrucco, Yoonji Eum, Xinan Wang, Raymond Paranal, Haiyun Wang, Mika Lin, Heidi M. Haikala, Jiaqi Li, Yue Xu, Joao Victor Alessi, Chhayheng Chhoeu, Amanda J. Redig, Jens Köhler, Kshiti H. Dholakia, Yunhan Chen, Elodie Richard, Marie-Julie Nokin, David Santamaria, Prafulla C. Gokhale, Mark M. Awad, Pasi A. Jänne, and Chiara Ambrogio

Subjects
Mitogen-Activated Protein Kinase Kinases, Cancer Research, Kelch-Like ECH-Associated Protein 1, Lung Neoplasms, NF-E2-Related Factor 2, Carcinoma, digestive system diseases, respiratory tract diseases, Proto-Oncogene Proteins p21(ras), Oncology, Carcinoma, Non-Small-Cell Lung, Mutation, Humans, Protein Isoforms, Non-Small-Cell Lung, neoplasms
Abstract

Purpose:Activating missense mutations of KRAS are the most frequent oncogenic driver events in lung adenocarcinoma (LUAD). However, KRAS isoforms are highly heterogeneous, and data on the potential isoform-dependent therapeutic vulnerabilities are still lacking.Experimental Design:We developed an isogenic cell-based platform to compare the oncogenic properties and specific therapeutic actionability of KRAS-mutant isoforms. In parallel, we analyzed clinicopathologic and genomic data from 3,560 patients with non–small cell lung cancer (NSCLC) to survey allele-specific features associated with oncogenic KRAS mutations.Results:In isogenic cell lines expressing different mutant KRAS isoforms, we identified isoform-specific biochemical, biological, and oncogenic properties both in vitro and in vivo. These exclusive features correlated with different therapeutic responses to MEK inhibitors, with KRAS G12C and Q61H mutants being more sensitive compared with other isoforms. In vivo, combined KRAS G12C and MEK inhibition was more effective than either drug alone. Among patients with NSCLCs that underwent comprehensive tumor genomic profiling, STK11 and ATM mutations were significantly enriched among tumors harboring KRAS G12C, G12A, and G12V mutations. KEAP1 mutation was significantly enriched among KRAS G12C and KRAS G13X LUADs. KRAS G13X-mutated tumors had the highest frequency of concurrent STK11 and KEAP1 mutations. Transcriptomic profiling revealed unique patterns of gene expression in each KRAS isoform, compared with KRAS wild-type tumors.Conclusions:This study demonstrates that KRAS isoforms are highly heterogeneous in terms of concurrent genomic alterations and gene-expression profiles, and that stratification based on KRAS alleles should be considered in the design of future clinical trials.

Published
2022

42. Annealing High Aspect Ratio Microgels into Macroporous 3D Scaffolds Allows for Higher Porosities and Effective Cell Migration

Author

Alisa C. Suturin, Andreas J. D. Krüger, Kathrin Neidig, Nina Klos, Nina Dolfen, Michelle Bund, Till Gronemann, Rebecca Sebers, Anna Manukanc, Ghazaleh Yazdani, Yonca Kittel, Dirk Rommel, Tamás Haraszti, Jens Köhler, and Laura De Laporte

Subjects
Biomaterials, Biomedical Engineering, Pharmaceutical Science
Abstract

Advanced healthcare materials 11(24), 2200989 (2022). doi:10.1002/adhm.202200989 special issue: "Special Issue:Biofabrication Applications", Published by Wiley-VCH, Weinheim

Published
2022

45. Insights into Ergochromes of the Plant Pathogen

Author

Friederike, Lünne, Jens, Köhler, Christina, Stroh, Lena, Müller, Constantin G, Daniliuc, Christian, Mück-Lichtenfeld, Ernst-Ulrich, Würthwein, Melanie, Esselen, Hans-Ulrich, Humpf, and Svetlana A, Kalinina

Subjects
Molecular Structure, Xanthenes, Topoisomerase Inhibitors, Xanthones, Humans, Hep G2 Cells, Claviceps
Published
2021

46. Die Notfallapotheke des Projektmanagements

Author

Jens Köhler

Abstract

Die Kolumne „Ehrlich und Priesberg“ möchte mit unterhaltsamen Dialogen rund um das Thema „Mensch – Kommunikation, Verhalten, Entscheidungen“ Denkanstöße für den PM-Alltag geben.

Published
2021

48. Sanierung des Rücklaufschlammkanals der Kläranlage Frankfurt-Sindlingen

Author

Jens Köhler Ferreira

Abstract

Instandsetzungen der Betoninfrastruktur verfahrenstechnischer Einrichtungen auf Kläranlagen sind komplex. Der langjährige Schutz sanierter Bauteile, wie auf der KA Frankfurt-Sindelfingen, ist deshalb ökonomisch und ökologisch entscheidend

Published
2021

49. Bewusst inkompetent - manchmal von Vorteil

Author

Jens Köhler

Abstract

Die Kolumne „Ehrlich und Priesberg“ möchte mit unterhaltsamen Dialogen rund um das Thema „Mensch – Kommunikation, Verhalten, Entscheidungen“ Denkanstöße für den PM-Alltag geben.

Published
2022

50. MPS1 inhibition primes immunogenicity of KRAS-LKB1 mutant lung cancer

Author

Shunsuke Kitajima, Tetsuo Tani, Benjamin F. Springer, Marco Campisi, Tatsuya Osaki, Koji Haratani, Minyue Chen, Erik H. Knelson, Navin R. Mahadevan, Jessica Ritter, Ryohei Yoshida, Jens Köhler, Atsuko Ogino, Ryu-Suke Nozawa, Shriram K. Sundararaman, Tran C. Thai, Mizuki Homme, Brandon Piel, Sophie Kivlehan, Bonje N. Obua, Connor Purcell, Mamiko Yajima, Thanh U. Barbie, Patrick H. Lizotte, Pasi A. Jänne, Cloud P. Paweletz, Prafulla C. Gokhale, and David A. Barbie

Subjects
Proto-Oncogene Proteins p21(ras), Cancer Research, Genes, ras, Lung Neoplasms, Oncology, Humans, Decitabine, Ligands
Abstract

KRAS-LKB1 (KL) mutant lung cancers silence STING owing to intrinsic mitochondrial dysfunction, resulting in T cell exclusion and resistance to programmed cell death (ligand) 1 (PD-[L]1) blockade. Here we discover that KL cells also minimize intracellular accumulation of 2'3'-cyclic GMP-AMP (2'3'-cGAMP) to further avoid downstream STING and STAT1 activation. An unbiased screen to co-opt this vulnerability reveals that transient MPS1 inhibition (MPS1i) potently re-engages this pathway in KL cells via micronuclei generation. This effect is markedly amplified by epigenetic de-repression of STING and only requires pulse MPS1i treatment, creating a therapeutic window compared with non-dividing cells. A single course of decitabine treatment followed by pulse MPS1i therapy restores T cell infiltration in vivo, enhances anti-PD-1 efficacy, and results in a durable response without evidence of significant toxicity.

Published
2021

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