Your search keyword '"Knapp S."' showing total 32,274 results

151. Design, Synthesis, and Biochemical Evaluation of Novel MLK3 Inhibitors: A Target Hopping Example.

Author

Sander P, Schwalm MP, Krämer A, Elson L, Rasch A, Masberg B, Selig R, Sievers-Engler A, Lämmerhofer M, Müller S, Knapp S, Albrecht W, and Laufer SA

Subjects

Humans, Structure-Activity Relationship, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Drug Design

Abstract

The human kinome has tremendous medical potential. In the past decade, mixed-lineage protein kinase 3 (MLK3) has emerged as an interesting and druggable target in oncogenic signaling. The important role of MLK3 has been demonstrated in several types of cancer. In a target hopping example we started with the focal adhesion kinase (FAK) inhibitor PF-431396 ( 10 ), which shows off-target activity toward MLK3. We were able to develop highly active compounds in the single digit nanomolar range for MLK3. Furthermore, we achieved a dramatic shift in selectivity from FAK to MLK3. Here we present a new chemical class of MLK3 inhibitors, including our lead compound 37 with an outstanding IC 50 value of <1 nM in a biochemical MLK3 assay while simultaneously exhibiting kinome-wide selectivity.

Published

2025

152. Development and Discovery of a Selective Degrader of Casein Kinases 1 δ/ε.

Author

Haag A, Němec V, Janovská P, Bartošíková J, Adhikari B, Müller J, Schwalm MP, Čada Š, Ohmayer U, Daub H, Kim Y, Born F, Wolf E, Bryja V, and Knapp S

Subjects

Humans, Drug Discovery, Casein Kinase 1 epsilon antagonists & inhibitors, Casein Kinase 1 epsilon metabolism, Casein Kinase Idelta antagonists & inhibitors, Casein Kinase Idelta metabolism, Proteolysis drug effects, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors metabolism

Abstract

Members of the casein kinase 1 (CK1) family have emerged as key regulators of cellular signaling and as potential drug targets. Functional annotation of the 7 human isoforms would benefit from isoform-selective inhibitors, allowing studies on the role of these enzymes in normal physiology and disease pathogenesis. However, due to significant sequence homology within the catalytic domain, isoform selectivity is difficult to achieve with conventional small molecules. Here, we used a PROTAC (Proteolysis TArgeting Chimeras) approach to develop a highly selective degrader AH078 ( 37 ) targeting CK1δ and CK1ε with excellent selectivity over the highly related CK1α isoform. The developed PROTAC, AH078 ( 37 ) selectively degraded CK1δ and CK1ε with a DC 50 of 200 nM. Characterization of AH078 ( 37 ) revealed a VHL and Ubiquitin-dependent degradation mechanism. Thus, AH078 ( 37 ) represents a versatile chemical tool to study CK1δ and CK1ε function in cellular systems.

Published

2025

153. The C-terminal PHDVC5HCH tandem domain of NSD2 is a combinatorial reader of unmodified H3K4 and tri-methylated H3K27 that regulates transcription of cell adhesion genes in multiple myeloma.

Author

Berardi A, Kaestner CL, Ghitti M, Quilici G, Cocomazzi P, Li J, Ballabio F, Zucchelli C, Knapp S, Licht JD, and Musco G

Subjects

Humans, Methylation, Repressor Proteins metabolism, Repressor Proteins genetics, Repressor Proteins chemistry, Protein Domains, Cell Line, Tumor, Gene Expression Regulation, Neoplastic, Transcription, Genetic, Molecular Dynamics Simulation, Chromatin metabolism, Multiple Myeloma genetics, Multiple Myeloma metabolism, Histone-Lysine N-Methyltransferase genetics, Histone-Lysine N-Methyltransferase metabolism, Histone-Lysine N-Methyltransferase chemistry, Histones metabolism, Histones genetics, Cell Adhesion genetics

Abstract

Histone methyltransferase NSD2 (MMSET) overexpression in multiple myeloma (MM) patients plays an important role in the development of this disease subtype. Through the expansion of transcriptional activating H3K36me2 and the suppression of repressive H3K27me3 marks, NSD2 activates an aberrant set of genes that contribute to myeloma growth, adhesive and invasive activities. NSD2 transcriptional activity also depends on its non-catalytic domains, which facilitate its recruitment to chromatin through histone binding. In this study, using NMR, ITC and molecular dynamics simulations, we show that the tandem PHD domain of NSD2 (PHDVC5HCHNSD2) is a combinatorial reader of unmodified histone H3K4 and tri-methylated H3K27 (H3K27me3). This is the first PHD tandem cassette known to decode the methylation status of H3K27. Importantly, in a NSD2-dependent MM cellular model, we show that expression of NSD2 mutants, engineered to disrupt the interaction between H3K27me3 and PHDVC5HCH, display in comparison to wild-type NSD2: incomplete loss of H3K27 methylation throughout the genome, decreased activation of adhesive properties and cell adhesion genes, and a decrease of the corresponding H3K27ac signal at promoters. Collectively, these data suggest that the PHDVC5HCH domain of NSD2 plays an important role in modulating gene expression and chromatin modification, providing new opportunities for pharmacological intervention., (© The Author(s) 2024. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2025

154. Alternative splicing in the DBD linker region of p63 modulates binding to DNA and iASPP in vitro.

Author

Lotz R, Osterburg C, Chaikuad A, Weber S, Akutsu M, Machel AC, Beyer U, Gebel J, Löhr F, Knapp S, Dobbelstein M, Lu X, and Dötsch V

Subjects

Humans, Tumor Suppressor Proteins metabolism, Tumor Suppressor Proteins genetics, Protein Isoforms metabolism, Protein Isoforms genetics, Transcription Factors metabolism, Transcription Factors genetics, Binding Sites, Amino Acid Sequence, Trans-Activators metabolism, Trans-Activators genetics, Trans-Activators chemistry, Protein Domains, Animals, Alternative Splicing genetics, Protein Binding, DNA metabolism, DNA genetics, Repressor Proteins metabolism, Repressor Proteins genetics, Intracellular Signaling Peptides and Proteins metabolism, Intracellular Signaling Peptides and Proteins genetics

Abstract

The transcription factor p63 is expressed in many different isoforms as a result of differential promoter use and splicing. Some of these isoforms have very specific physiological functions in the development and maintenance of epithelial tissues and surveillance of genetic integrity in oocytes. The ASPP family of proteins is involved in modulating the transcriptional activity of the p53 protein family members, including p63. In particular, iASPP plays an important role in the development and differentiation of epithelial tissues. Here we characterize the interaction of iASPP with p63 and show that it binds to the linker region between the DNA binding domain and the oligomerization domain. We further demonstrate that this binding site is removed in a splice variant of p63 where a stretch of five amino acids is replaced with a single alanine residue. This stretch contains a degenerate class II SH3 domain binding motif that is responsible for interaction with iASPP, as well as two positively charged amino acids. Moreover, the concomitant loss of the charged amino acids in the alternatively spliced version decreases the affinity of p63 to its cognate DNA element two- to threefold. mRNAs encoding full-length p63, as well as its alternatively spliced version, are present in all tissues that we investigated, albeit in differing ratios. We speculate that, through the formation of hetero-complexes of both isoforms, the affinity to DNA, as well as the interaction with iASPP, can be fine-tuned in a tissue-specific manner., Competing Interests: Competing interests: The authors declare no competing interests. Ethical statement: All methods were performed in accordance with the relevant guidelines and regulations. As this is an in vitro study without human patients or animals involved no ethics committee approval was required. The human cDNA from ten different tissues was purchased directly from the company Zyagen without any connection to identifiable human patients., (© 2025. The Author(s).)

Published

2025

155. Thieno[3,2-b]pyridine: Attractive scaffold for highly selective inhibitors of underexplored protein kinases with variable binding mode.

Author

Moyano PM, Kubina T, Paruch ŠO, Jarošková A, Novotný J, Skočková V, Ovesná P, Suchánková T, Prokofeva P, Kuster B, Šmída M, Chaikuad A, Krämer A, Knapp S, Souček K, and Paruch K

Abstract

Protein kinases are key regulators of numerous biological processes and aberrant kinase activity can cause various diseases, particularly cancer. Herein, we report the identification of new series of highly selective kinase inhibitors based on the thieno[3,2-b]pyridine scaffold. The weak interaction of the thieno[3,2-b]pyridine core with the kinase hinge region allows for profoundly different binding modes all of which maintain high kinome-wide selectivity, as illustrated by the isomers MU1464 and MU1668. Thus, this core structure provides a template of ATP-competitive but not ATP-mimetic inhibitors that are anchored at the kinase back pocket. Mapping the chemical space around the central thieno[3,2-b]pyridine pharmacophore afforded highly selective inhibitors of the kinase Haspin, exemplified by the compound MU1920 that fulfils criteria for a quality chemical probe and is suitable for use in in vivo applications. However, despite the role of Haspin in mitosis, the inhibition of Haspin alone was not sufficient to elicit cytotoxic effect in cancer cells. The thieno[3,2-b]pyridine scaffold can be used in a broader context, as a basis of inhibitors targeting other underexplored protein kinases, such as CDKLs., (© 2024 The Author(s). Angewandte Chemie International Edition published by Wiley-VCH GmbH.)

Published

2025

156. Chaplain care for health care colleagues: a scoping review.

Author

Knapp S, Schaefer B, Stratton RG, Usset TJ, K Yadav S, and Fitchett G

Subjects

Humans, Clergy, Chaplaincy Service, Hospital, Professional Role, Pastoral Care, COVID-19, Health Personnel psychology

Abstract

In addition to supporting patients and their loved ones at critical times, chaplains have long understood that caring for their health care colleagues is an important part of their practice. The Covid-19 pandemic prompted conversations among chaplains about how best to address the stress they were observing in health care workers. Our team conducted a scoping review in PubMed and CINAHL of peer reviewed literature describing chaplaincy care for health care workers. We started with 364 unique articles and found 59 that met criteria for the review. Five themes surfaced in analysis of these articles, with two themes emerging as most important: (1) descriptions of care for staff as part of the chaplain's role, especially when staff are making difficult decisions and (2) reports of the effects of chaplain care for staff, both indirect and direct. We discovered that research was limited, and more research is needed regarding chaplain care for health care colleagues.

Published

2025

157. Thoughts for the future.

Author

Alkhalaf LM, Arrowsmith C, Balskus EP, Bergamini G, Bhandari R, Chang CJ, Chen P, Chen X, Ciulli A, Cricco JA, Davis BG, Delbianco M, Dudareva N, Dueber E, Ferguson F, de Giuseppe PO, Hamachi I, Hammond MC, Hatzios SK, Do Heo W, Janet JP, Kamat SS, Knapp S, Krishnan Y, Lang K, Laraia L, Leveson-Gower RB, Li XD, Liu DR, Liu MF, London N, Mahanta N, Mayor-Ruiz C, Muir T, Murakami MT, Rhee HW, Robers M, Satz A, Schulman BA, Shen B, Shoichet B, Strauss E, Suzuki T, Tiwary P, Waldmann H, Ward TR, Weeks A, Weerapana E, and Winter G

Published

2025

158. Molecular basis of JAK kinase regulation guiding therapeutic approaches: Evaluating the JAK3 pseudokinase domain as a drug target.

Author

Virtanen A, Kettunen V, Musta K, Räkköläinen V, Knapp S, Haikarainen T, and Silvennoinen O

Abstract

Janus kinases (JAK1-3, TYK2) are critical mediators of cytokine signaling and their role in hematological and inflammatory and autoimmune diseases has sparked widespread interest in their therapeutic targeting. JAKs have unique tandem kinase structure consisting of an active tyrosine kinase domain adjacent to a pseudokinase domain that is a hotspot for pathogenic mutations. The development of JAK inhibitors has focused on the active kinase domain and the developed drugs have demonstrated good clinical efficacy but due to off-target inhibition cause also side-effects and carry a black box warning limiting their use. Our understanding of the regulatory function of the pseudokinase domain in physiological and pathological signaling has improved substantially. The pseudokinase domain maintains the inactive state of JAKs in the absence of cytokine stimulation but it has also a key role in physiological and mutation-driven activation process. Furthermore, the pseudokinase domain has favourable structural characteristics for selective targeting of cytokine signaling, such as unique mode of ATP-binding, and the first pseudokinase targeting inhibitor for TYK2 has been approved for clinical use. Here we describe the recent functional and structural knowledge of JAK signaling and their therapeutic targeting, and present data evaluating the druggability of the JAK3 pseudokinase domain., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Olli Silvennoinen reports financial support was provided by Research Council of Finland. Teemu Haikarainen reports financial support was provided by Research Council of Finland. Olli Silvennoinen reports financial support was provided by Sigrid Jusélius Foundation. Olli Silvennoinen reports financial support was provided by Cancer Foundation Finland. Teemu Haikarainen reports financial support was provided by The Paulo Foundation. Olli Silvennoinen reports financial support was provided by Tampere Tuberculosis Foundation. Teemu Haikarainen reports financial support was provided by Tampere Tuberculosis Foundation. Olli Silvennoinen reports financial support was provided by Competitive Research Funding of the Tampere University Hospital. Olli Silvennoinen reports a relationship with Ajax Therapeutics that includes: board membership and equity or stocks. Olli Silvennoinen has patent #Novel function of JAK kinases (US 8841078, AU, 2011214254, CAN 2789186, EPO 11741946.5) issued to GENON BIOTECHNOLOGIES Oy. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2024

159. DARPins as a novel tool to detect and degrade p73.

Author

Münick P, Zielinski J, Strubel A, Gutfreund N, Dreier B, Schaefer JV, Schäfer B, Gebel J, Osterburg C, Chaikuad A, Knapp S, Plückthun A, and Dötsch V

Subjects

Humans, Ubiquitin-Protein Ligases metabolism, Protein Binding, Tumor Suppressor Protein p53 metabolism, Proteolysis, Tumor Protein p73 metabolism

Abstract

The concept of Targeted Protein Degradation (TPD) has been introduced as an attractive alternative to the development of classical inhibitors. TPD can extend the range of proteins that can be pharmacologically targeted beyond the classical targets for small molecule inhibitors, as a binding pocket is required but its occupancy does not need to lead to inhibition. The method is based on either small molecules that simultaneously bind to a protein of interest and to a cellular E3 ligase and bring them in close proximity (molecular glue) or a bi-functional molecule synthesized from the chemical linkage of a target protein-specific small molecule and one that binds to an E3 ligase (Proteolysis Targeting Chimeras (PROTAC)). The further extension of this approach to bioPROTACs, in which a small protein-based binding module is fused directly to an E3 ligase or an E3 ligase adaptor protein, makes virtually all proteins amenable to targeted degradation, as this method eliminates the requirement for binding pockets for small molecules. Designed Ankyrin Repeat Proteins (DARPins) represent a very attractive class of small protein-based binding modules that can be used for the development of bioPTOTACS. Here we describe the characterization of two DARPins generated against the oligomerization domain and the SAM domain of the transcription factor p73, a member of the p53 protein family. The DARPins can be used for (isoform-)selective pulldown experiments both in cell culture as well as primary tissue lysates. We also demonstrate that they can be used for staining in cell culture experiments. Fusing them to the speckle type POZ protein (SPOP), an adaptor protein for cullin-3 E3 ligase complexes, yields highly selective and effective degraders. We demonstrate that selective degradation of the ΔNp73α isoform reactivates p53., Competing Interests: Competing interests: Andreas Plückthun is a cofounder and shareholder of Molecular Partners AG, who are commercializing the DARPin technology. All other authors declare that they have no competing interests., (© 2024. The Author(s).)

Published

2024

160. Unlocking the potential: unveiling tyrphostins with Michael-reactive cyanoacrylate motif as promising inhibitors of human 5-lipoxygenase.

Author

Molitor M, Menge A, Mandel S, George S, Müller S, Knapp S, Hofmann B, Steinhilber D, and Häfner AK

Subjects

Humans, Cyanoacrylates pharmacology, Cyanoacrylates chemistry, Neutrophils metabolism, Neutrophils drug effects, Arachidonate 5-Lipoxygenase metabolism, Lipoxygenase Inhibitors pharmacology, Tyrphostins pharmacology

Abstract

Human 5-lipoxygenase (5-LO) is the key enzyme in the biosynthesis of leukotrienes, mediators of the innate immune system that also play an important role in inflammatory diseases and cancer. In this study, we present compounds, containing a Michael-reactive cyanoacrylate moiety as potent inhibitors of 5-LO. Representatives of the tyrosine kinase inhibitor family called tyrphostins, structurally related to known 5-LO inhibitors, were screened for their 5-LO inhibitory properties using recombinant human 5-LO, intact human PMNL (polymorphonuclear leukocytes), and PMNL homogenates. Their mode of action was characterized by the addition of glutathione, using a fourfold cysteine 5-LO mutant and mass spectrometry analysis. SAR studies revealed several members of the tyrphostin family containing a Michael-reactive cyanoacrylate to efficiently inhibit 5-LO. We identified degrasyn (IC 50 0.11 µM), tyrphostin A9 (IC 50 0.8 µM), AG879 (IC 50 78 nM), and AG556 (IC 50 64 nM) as potent 5-LO inhibitors. Mass spectrometry analysis revealed that degrasyn and AG556 covalently bound to up to four cysteines, including C416 and/or C418 which surround the substrate entry site. Furthermore, the 5-LO inhibitory effect of degrasyn was remarkably impaired by the addition of glutathione or by the mutation of cysteines to serines at the surface of 5-LO. We successfully identified several tyrphostins as potent inhibitors of human 5-LO. Degrasyn and AG556 were able to covalently bind to 5-LO via their cyanoacrylate moiety. This provides a promising mechanism for targeting 5-LO by Michael acceptors, leading to new therapeutic opportunities in the field of inflammation and cancer., Competing Interests: Declarations. Competing Interests: The authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

161. Non-inferiority of hybrid outpatient telerehabilitation for patients with back pain: 3-month follow-up of a randomized controlled trial.

Author

Albers R, Lemke S, Fauser D, Knapp S, Krischak G, and Bethge M

Subjects

Humans, Male, Female, Middle Aged, Adult, Follow-Up Studies, Germany, Aged, Adolescent, Pain Measurement, Treatment Outcome, Telerehabilitation, Back Pain rehabilitation

Abstract

Background: International studies identified comparable or better effects for telerehabilitation compared with face-to-face rehabilitation or no rehabilitation in people with back pain. In German rehabilitation centers, a standardized back school for patients with back pain is provided usually face-to-face as part of a multimodal rehabilitation program., Aim: To examine the non-inferiority of a three-week, digitally assisted, multimodal rehabilitation that applies a digital version of a standardized back school (intervention group [IG]) against the same rehabilitation program applying the back school face-to-face (control group [CG])., Design: Our study was a non-blinded multicenter randomized controlled trial. Recruitment was conducted from 2022 to 2023. We analyzed outcomes at the end of rehabilitation and 3 months later., Setting: Implementation of the study and enrollment of participants was conducted in 8 German outpatient rehabilitation centers., Population: Rehabilitants aged 18-65 years with back pain were included., Methods: 284 patients with back pain were randomized into the IG or CG using computer-generated block randomization. We excluded 14 patients as they withdrew their consent and requested removal of their data. We finally included 270 patients (IG: N.=127, CG: N.=143). The primary outcome was self-reported pain self-efficacy (10-60 points). Secondary outcomes were, amongst others, current health status and pain., Results: Our primary adjusted intention-to-treat analysis demonstrated that hybrid digitally assisted rehabilitation was non-inferior to face-to-face rehabilitation at the end of rehabilitation (b=-0.55; 95% CI=-2.75 to ∞) and at the 3-month follow-up (b=0.24; 95% CI=-2.86 to ∞). These results were in line with a non-adjusted intention-to-treat analysis, an adjusted complete case analysis, and an adjusted per-protocol analysis. Secondary outcomes were tested for superiority. Our primary adjusted intention-to-treat analysis found no significant group differences in the secondary outcomes., Conclusions: This study provides evidence that hybrid digitally assisted rehabilitation in patients with back pain is a sound alternative to face-to-face rehabilitation in an outpatient rehabilitation setting., Clinical Rehabilitation Impact: Hybrid digitally assisted rehabilitation can improve flexibility and access to rehabilitation. Further studies should examine which components and which time frame of rehabilitation can be digitized without any loss of effectiveness.

Published

2024

162. Reseña de 'FLORA MESOAMÉRICANA VOLUMEN 4, PARTE 1 CUCURBITACEAE A POLEMONIACEAE' de DAVIDSE, G., SOUSA S., M. KNAPP, S. Y CHIANG, F. EDS

Author

Rosaura Grether

Subjects

Biología

Published

2011

163. Nichtunterlegenheit einer hybriden ambulanten orthopädischen Rehabilitation: 3-Monats-Ergebnisse einer randomisierten kontrollierten Studie

Author

Albers, R, Lemke, S, Fauser, D, Knapp, S, Krischak, G, Bethge, M, Albers, R, Lemke, S, Fauser, D, Knapp, S, Krischak, G, and Bethge, M

Published

2024

164. KNAPP, S. and PRESS, J. R. The gilded canopy. Botanical ceiling panels of The Natural History Museum

Author

Nelson, E. Charles, primary

Published

2006

165. Knapp, S. Potted histories: an artistic voyage through plant exploration

Author

Nelson, E. Charles, primary

Published

2004

166. Toward target 2035: EUbOPEN - a public-private partnership to enable & unlock biology in the open.

Author

Tredup C, Ackloo S, Beck H, Brown PJ, Bullock AN, Ciulli A, Dikic I, Edfeldt K, Edwards AM, Elkins JM, Farin HF, Fon EA, Gstaiger M, Günther J, Gustavsson AL, Häberle S, Isigkeit L, Huber KVM, Kotschy A, Krämer O, Leach AR, Marsden BD, Matsui H, Merk D, Montel F, Mulder MPC, Müller S, Owen DR, Proschak E, Röhm S, Stolz A, Sundström M, von Delft F, Willson TM, Arrowsmith CH, and Knapp S

Abstract

Target 2035 is a global initiative that seeks to identify a pharmacological modulator of most human proteins by the year 2035. As part of an ongoing series of annual updates of this initiative, we summarise here the efforts of the EUbOPEN project whose objectives and results are making a strong contribution to the goals of Target 2035. EUbOPEN is a public-private partnership with four pillars of activity: (1) chemogenomic library collections, (2) chemical probe discovery and technology development for hit-to-lead chemistry, (3) profiling of bioactive compounds in patient-derived disease assays, and (4) collection, storage and dissemination of project-wide data and reagents. The substantial outputs of this programme include a chemogenomic compound library covering one third of the druggable proteome, as well as 100 chemical probes, both profiled in patient derived assays, as well as hundreds of data sets deposited in existing public data repositories and a project-specific data resource for exploring EUbOPEN outputs., Competing Interests: There are no conflicts to declare., (This journal is © The Royal Society of Chemistry.)

Published

2024

167. Carfilzomib-associated thrombotic microangiopathy: clinical features and outcomes.

Author

Joseph A, Harel S, Mesnard L, Rafat C, Knapp S, Rumpler A, Philipponnet C, Barba C, Rebibou JM, Buob D, Hertig A, Vargaftig J, Halimi JM, Arnulf B, Bretaud AS, Joly B, Grangé S, and Coppo P

Subjects

Humans, Male, Female, Middle Aged, Aged, Acute Kidney Injury chemically induced, Acute Kidney Injury etiology, COVID-19 complications, Antibodies, Monoclonal, Humanized therapeutic use, Antibodies, Monoclonal, Humanized adverse effects, Multiple Myeloma drug therapy, Adult, Proteasome Inhibitors therapeutic use, Proteasome Inhibitors adverse effects, SARS-CoV-2, Retrospective Studies, Aged, 80 and over, Thrombotic Microangiopathies etiology, Thrombotic Microangiopathies chemically induced, Thrombotic Microangiopathies drug therapy, Oligopeptides therapeutic use, Oligopeptides adverse effects

Abstract

Background: Carfilzomib, a new proteasome inhibitor indicated for patients with relapsed/refractory myeloma, has been associated with cases of thrombotic microangiopathy (CFZ-TMA). The role of variants in the complement alternative pathway and therapeutic potential of complement blockade with eculizumab remain to be determined., Methods: We report 37 cases of CFZ-TMA recorded in the French reference center for TMA with their clinical characteristics, genetic analysis and outcome according to treatments., Results: A trigger was identified in more than half of cases, including eight influenza and five severe acute respiratory syndrome coronavirus-2 cases. All patients presented with acute kidney injury (AKI) [KDIGO stage 3 in 31 (84%) patients] while neurological (n = 13, 36%) and cardiac (n = 7, 19%) damage were less frequent. ADAMTS13 (a disintegrin and metalloprotease with thrombospondin type I repeats-13) and complement activity were normal (n = 28 and 18 patients tested) and no pathogenic variant in the alternative complement pathway was found in 7 patients tested. TMA resolved in most (n = 34, 94%) patients but 12 (44%) still displayed stage 3 AKI at discharge. Nineteen (51%) patients were treated with therapeutic plasma exchange, 14 (38%) patients received corticosteroids and 18 (50%) were treated with eculizumab. However, none of these treatments demonstrated a significant impact on outcomes., Conclusion: This study is the largest case series of CFZ-TMA since its approval in 2012. Patients present with severe AKI and experience frequent sequelae. Complement variants and blockade therapy do not seem to play a role in the pathophysiology and prognosis of the disease., (© The Author(s) 2024. Published by Oxford University Press on behalf of the ERA.)

Published

2024

168. Critical assessment of LC3/GABARAP ligands used for degrader development and ligandability of LC3/GABARAP binding pockets.

Author

Schwalm MP, Dopfer J, Kumar A, Greco FA, Bauer N, Löhr F, Heering J, Cano-Franco S, Lechner S, Hanke T, Jaser I, Morasch V, Lenz C, Fearon D, Marples PG, Tomlinson CWE, Brunello L, Saxena K, Adams NBP, von Delft F, Müller S, Stolz A, Proschak E, Kuster B, Knapp S, and Rogov VV

Subjects

Ligands, Humans, Binding Sites, Protein Binding, Autophagy, Crystallography, X-Ray, Microtubule-Associated Proteins metabolism, Microtubule-Associated Proteins chemistry, Apoptosis Regulatory Proteins metabolism, Apoptosis Regulatory Proteins chemistry, Molecular Docking Simulation, Adaptor Proteins, Signal Transducing metabolism, Adaptor Proteins, Signal Transducing chemistry, Autophagosomes metabolism

Abstract

Recent successes in developing small molecule degraders that act through the ubiquitin system have spurred efforts to extend this technology to other mechanisms, including the autophagosomal-lysosomal pathway. Therefore, reports of autophagosome tethering compounds (ATTECs) have received considerable attention from the drug development community. ATTECs are based on the recruitment of targets to LC3/GABARAP, a family of ubiquitin-like proteins that presumably bind to the autophagosome membrane and tether cargo-loaded autophagy receptors into the autophagosome. In this work, we rigorously tested the target engagement of the reported ATTECs to validate the existing LC3/GABARAP ligands. Surprisingly, we were unable to detect interaction with their designated target LC3 using a diversity of biophysical methods. Intrigued by the idea of developing ATTECs, we evaluated the ligandability of LC3/GABARAP by in silico docking and large-scale crystallographic fragment screening. Data based on approximately 1000 crystal structures revealed that most fragments bound to the HP2 but not to the HP1 pocket within the LIR docking site, suggesting a favorable ligandability of HP2. Through this study, we identified diverse validated LC3/GABARAP ligands and fragments as starting points for chemical probe and ATTEC development., Competing Interests: Competing interests: The authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

169. Exploring biodiversity through museomics.

Author

Davis CC and Knapp S

Published

2024

170. Oxadiazolone-Based Aromatic Annulations: A Nitrenoid Precursor for Tricyclic Aminoheterocycles.

Author

Zhu WF, Franz HM, Krämer A, Duman E, Empel C, Göbel MW, Koenigs RM, Knapp S, Hiesinger K, Proschak E, and Hernandez-Olmos V

Subjects

Molecular Structure, Heterocyclic Compounds chemistry, Heterocyclic Compounds chemical synthesis, Cyclization, Oxadiazoles chemistry

Abstract

Nitrogen-containing heterocycles are present in most approved drugs, reflecting the significance of their synthetic strategies. By utilizing oxadiazolone as a nitrenoid (nitrene-like) precursor, we have developed a general strategy for the annulation with nucleophilic heterocycles to access various polycyclic aminoheterocycles. We have discovered that 2-pyrryl-substituted substrates undergo a rearrangement, which indicates a spirocyclization-migration pathway. Given their fluorescence and biological activity as kinase hinge binders, these fragment-like aminoheterocycles represent potential starting points for applications in chemical biology and drug discovery.

Published

2024

171. KNAPP, S. Footsteps in the forest. The Natural History Museum, London: 1999. Pp vi, 90; illustrated (67 monochrome plates, maps). Price £ 16.95 (hardback). ISBN 0-565-09143-3.

Author

WALKER, TREVOR, primary

Published

2001

172. Type-II kinase inhibitors that target Parkinson's Disease-associated LRRK2.

Author

Raig ND, Surridge KJ, Sanz-Murillo M, Dederer V, Krämer A, Schwalm MP, Elson L, Chatterjee D, Mathea S, Hanke T, Leschziner AE, Reck-Peterson SL, and Knapp S

Abstract

Aberrant increases in kinase activity of leucine-rich repeat kinase 2 (LRRK2) are associated with Parkinson's disease (PD). Numerous LRRK2-selective type-I kinase inhibitors have been developed and some have entered clinical trials. In this study, we present the first LRRK2-selective type-II kinase inhibitors. Targeting the inactive conformation of LRRK2 is functionally distinct from targeting the active-like conformation using type-I inhibitors. We designed these inhibitors using a combinatorial chemistry approach fusing selective LRRK2 type-I and promiscuous type-II inhibitors by iterative cycles of synthesis supported by structural biology and activity testing. Our current lead structures are selective and potent LRRK2 inhibitors. Through cellular assays, cryo-electron microscopy structural analysis, and in vitro motility assays, we show that our inhibitors stabilize the open, inactive kinase conformation. These new conformation-specific compounds will be invaluable as tools to study LRRK2's function and regulation, and expand the potential therapeutic options for PD.

Published

2024

173. Chem-CRISPR/dCas9FCPF: a platform for chemically induced epigenome editing.

Author

Altinbay M, Wang J, Chen J, Schäfer D, Sprang M, Blagojevic B, Wölfl S, Andrade-Navarro MA, Dikic I, Knapp S, and Cheng X

Subjects

Humans, Azepines pharmacology, Triazoles pharmacology, HEK293 Cells, Proto-Oncogene Proteins c-myc genetics, Proto-Oncogene Proteins c-myc metabolism, Cell Cycle Proteins genetics, Cell Cycle Proteins metabolism, Epigenome, CRISPR-Associated Protein 9 genetics, CRISPR-Associated Protein 9 metabolism, RNA, Guide, CRISPR-Cas Systems genetics, Bromodomain Containing Proteins, CRISPR-Cas Systems, Gene Editing methods, Transcription Factors genetics, Transcription Factors metabolism, Epigenesis, Genetic drug effects

Abstract

Epigenetic aberration is one of the major driving factors in human cancer, often leading to acquired resistance to chemotherapies. Various small molecule epigenetic modulators have been reported. Nonetheless, outcomes from animal models and clinical trials have underscored the substantial setbacks attributed to pronounced on- and off-target toxicities. To address these challenges, CRISPR/dCas9 technology is emerging as a potent tool for precise modulation of epigenetic mechanism. However, this technology involves co-expressing exogenous epigenetic modulator proteins, which presents technical challenges in preparation and delivery with potential undesirable side effects. Recently, our research demonstrated that Cas9 tagged with the Phe-Cys-Pro-Phe (FCPF)-peptide motif can be specifically targeted by perfluorobiphenyl (PFB) derivatives. Here, we integrated the FCPF-tag into dCas9 and established a chemically inducible platform for epigenome editing, called Chem-CRISPR/dCas9FCPF. We designed a series of chemical inhibitor-PFB conjugates targeting various epigenetic modulator proteins. Focusing on JQ1, a panBET inhibitor, we demonstrate that c-MYC-sgRNA-guided JQ1-PFB specifically inhibits BRD4 in close proximity to the c-MYC promoter/enhancer, thereby effectively repressing the intricate transcription networks orchestrated by c-MYC as compared with JQ1 alone. In conclusion, our Chem-CRISPR/dCas9FCPF platform significantly increased target specificity of chemical epigenetic inhibitors, offering a viable alternative to conventional fusion protein systems for epigenome editing., (© The Author(s) 2024. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2024

174. Nuclear receptor corepressor 1 controls regulatory T cell subset differentiation and effector function.

Author

Stolz V, de Freitas E Silva R, Rica R, Zhu C, Preglej T, Hamminger P, Hainberger D, Alteneder M, Müller L, Waldherr M, Waltenberger D, Hladik A, Agerer B, Schuster M, Frey T, Krausgruber T, Knapp S, Campbell C, Schmetterer K, Trauner M, Bergthaler A, Bock C, Boucheron N, and Ellmeier W

Subjects

Animals, Mice, Humans, Liver X Receptors metabolism, Liver X Receptors genetics, Mice, Inbred C57BL, Colitis immunology, Colitis genetics, T-Lymphocyte Subsets immunology, T-Lymphocyte Subsets metabolism, Mice, Knockout, T-Lymphocytes, Regulatory immunology, Nuclear Receptor Co-Repressor 1 metabolism, Nuclear Receptor Co-Repressor 1 genetics, Cell Differentiation

Abstract

FOXP3 + regulatory T cells (Treg cells) are key for immune homeostasis. Here, we reveal that nuclear receptor corepressor 1 (NCOR1) controls naïve and effector Treg cell states. Upon NCOR1 deletion in T cells, effector Treg cell frequencies were elevated in mice and in in vitro-generated human Treg cells. NCOR1-deficient Treg cells failed to protect mice from severe weight loss and intestinal inflammation associated with CD4 + T cell transfer colitis, indicating impaired suppressive function. NCOR1 controls the transcriptional integrity of Treg cells, since effector gene signatures were already upregulated in naïve NCOR1-deficient Treg cells while effector NCOR1-deficient Treg cells failed to repress genes associated with naïve Treg cells. Moreover, genes related to cholesterol homeostasis including targets of liver X receptor (LXR) were dysregulated in NCOR1-deficient Treg cells. However, genetic ablation of LXRβ in T cells did not revert the effects of NCOR1 deficiency, indicating that NCOR1 controls naïve and effector Treg cell subset composition independent from its ability to repress LXRβ-induced gene expression. Thus, our study reveals that NCOR1 maintains naïve and effector Treg cell states via regulating their transcriptional integrity. We also reveal a critical role for this epigenetic regulator in supporting the suppressive functions of Treg cells in vivo., Competing Interests: VS, Rd, RR, CZ, TP, PH, DH, MA, LM, MW, DW, AH, BA, MS, TF, TK, SK, CC, KS, MT, AB, CB, NB, WE No competing interests declared, (© 2024, Stolz, de Freitas e Silva et al.)

Published

2024

175. Synthesis and evaluation of chemical linchpins for highly selective CK2α targeting.

Author

Greco FA, Krämer A, Wahl L, Elson L, Ehret TAL, Gerninghaus J, Möckel J, Müller S, Hanke T, and Knapp S

Subjects

Humans, Structure-Activity Relationship, Molecular Structure, Dose-Response Relationship, Drug, Models, Molecular, Adenosine Triphosphate metabolism, Binding Sites, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Casein Kinase II antagonists & inhibitors, Casein Kinase II metabolism

Abstract

Casein kinase-2 (CK2) are serine/threonine kinases with dual co-factor (ATP and GTP) specificity, that are involved in the regulation of a wide variety of cellular functions. Small molecules targeting CK2 have been described in the literature targeting different binding pockets of the kinase with a focus on type I inhibitors such as the recently published chemical probe SGC-CK2-1. In this study, we investigated whether known allosteric inhibitors binding to a pocket adjacent to helix αD could be combined with ATP mimetic moieties defining a novel class of ATP competitive compounds with a unique binding mode. Linking both binding sites requires a chemical linking moiety that would introduce a 90-degree angle between the ATP mimetic ring system and the αD targeting moiety, which was realized using a sulfonamide. The synthesized inhibitors were highly selective for CK2 with binding constants in the nM range and low micromolar activity. While these inhibitors need to be further improved, the present work provides a structure-based design strategy for highly selective CK2 inhibitors., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Masson SAS.. All rights reserved.)

Published

2024

176. RUNX1 interacts with lncRNA SMANTIS to regulate monocytic cell functions.

Author

Weiss LM, Warwick T, Zehr S, Günther S, Wolf S, Schmachtel T, Izquierdo Ponce J, Pálfi K, Teichmann T, Schneider A, Stötzel J, Knapp S, Weigert A, Savai R, Rieger MA, Oellerich T, Wittig I, Oo JA, Brandes RP, and Leisegang MS

Subjects

Humans, Cell Adhesion genetics, Cell Differentiation, RNA, Long Noncoding genetics, RNA, Long Noncoding metabolism, Monocytes metabolism, Core Binding Factor Alpha 2 Subunit metabolism, Core Binding Factor Alpha 2 Subunit genetics

Abstract

Monocytes, the circulating macrophage precursors, contribute to diseases like atherosclerosis and asthma. Long non-coding RNAs (lncRNAs) have been shown to modulate the phenotype and inflammatory capacity of monocytes. We previously discovered the lncRNA SMANTIS, which contributes to cellular phenotype expression by controlling BRG1 in mesenchymal cells. Here, we report that SMANTIS is particularly highly expressed in monocytes and lost during differentiation into macrophages. Moreover, different types of myeloid leukemia presented specific SMANTIS expression patterns. Interaction studies revealed that SMANTIS binds RUNX1, a transcription factor frequently mutated in AML, primarily through its Alu-element on the RUNT domain. RNA-seq after CRISPR/Cas9-mediated deletion of SMANTIS or RUNX1 revealed an association with cell adhesion and both limited the monocyte adhesion to endothelial cells. Mechanistically, SMANTIS KO reduced RUNX1 genomic binding and altered the interaction of RUNX1 with EP300 and CBFB. Collectively, SMANTIS interacts with RUNX1 and attenuates monocyte adhesion, which might limit monocyte vascular egress., (© 2024. The Author(s).)

Published

2024

177. Elimination of mutant SWI/SNF complexes by protein quality control: new opportunities targeting aggressive rhabdoid tumours.

Author

Krämer A and Knapp S

Subjects

Humans, Chromosomal Proteins, Non-Histone genetics, Chromosomal Proteins, Non-Histone metabolism, Mutation, SMARCB1 Protein genetics, SMARCB1 Protein metabolism, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Rhabdoid Tumor genetics, Rhabdoid Tumor pathology, Transcription Factors genetics, Transcription Factors metabolism

Published

2024

178. Optimization of diastereomeric dihydropyridines as antimalarials.

Author

Van Horn KS, Zhao Y, Parvatkar PT, Maier J, Mutka T, Lacrue A, Brockmeier F, Ebert D, Wu W, Casandra DR, Namelikonda N, Yacoub J, Sigal M, Knapp S, Floyd D, Waterson D, Burrows JN, Duffy J, DeRisi JL, Kyle DE, Guy RK, and Manetsch R

Subjects

Structure-Activity Relationship, Animals, Mice, Stereoisomerism, Parasitic Sensitivity Tests, Molecular Structure, Dose-Response Relationship, Drug, Humans, Antimalarials pharmacology, Antimalarials chemistry, Antimalarials chemical synthesis, Dihydropyridines pharmacology, Dihydropyridines chemistry, Dihydropyridines chemical synthesis, Plasmodium falciparum drug effects

Abstract

The increase in research funding for the development of antimalarials since 2000 has led to a surge of new chemotypes with potent antimalarial activity. High-throughput screens have delivered several thousand new active compounds in several hundred series, including the 4,7-diphenyl-1,4,5,6,7,8-hexahydroquinolines, hereafter termed dihydropyridines (DHPs). We optimized the DHPs for antimalarial activity. Structure-activity relationship studies focusing on the 2-, 3-, 4-, 6-, and 7-positions of the DHP core led to the identification of compounds potent (EC 50  < 10 nM) against all strains of P. falciparum tested, including the drug-resistant parasite strains K1, W2, and TM90-C2B. Evaluation of efficacy of several compounds in vivo identified two compounds that reduced parasitemia by >75 % in mice 6 days post-exposure following a single 50 mg/kg oral dose. Resistance acquisition experiments with a selected dihydropyridine led to the identification of a single mutation conveying resistance in the gene encoding for Plasmodium falciparum multi-drug resistance protein 1 (PfMDR1). The same dihydropyridine possessed transmission blocking activity. The DHPs have the potential for the development of novel antimalarial drug candidates., Competing Interests: Declaration of competing interest The authors declare no conflicts of interest., (Copyright © 2024. Published by Elsevier Masson SAS.)

Published

2024

179. Changes to publication requirements made at the XVIII International Botanical Congress in Melbourne – What does e-publication mean for you?

Author

Knapp, S, Mcneill, J, Turland, Nicholas J, and BioStor

Published

2011

180. KNAPP, S. Footsteps in the forest. The Natural History Museum, London: 1999. Pp vi, 90; illustrated (67 monochrome plates, maps). Price £ 16.95 (hardback). ISBN 0-565-09143-3

Author

Trevor Walker

Subjects

Natural history, History, Anthropology, media_common.quotation_subject, Monochrome, Art history, Art, Agricultural and Biological Sciences (miscellaneous), media_common

Published

2001

181. Solanum coalitum (Solanaceae), a new endemic species from southern Ecuador

Author

Knapp, S and BioStor

Published

2007

182. H. MEUSEL; E. J. JÄGER (Hrsg.) Vergleichende Chorologie der Zentraleuropäischen Flora, Band III. Mit Beiträgen von S. BRÄUTIGAM; H.-D. KNAPP; S. RAUSCHERT (†); E. WEINERT. Unter Mitarbeit von D. SEIDEL und J. STÖLZER und Fachwissenschaftlern aus 20 Ländern. In zwei Teilen: Textband: 333 S.; Kartenband; Karten, Literatur und Gesamtregister, 688 S., Gustav Fischer Verlag, Jena, 1992. ISBN 3-334-00411-2. Preis (geb.) DM 560,—

Author

Fukarek, F., primary

Published

1994

183. KNAPP, S. and PRESS, J. R. The gilded canopy. Botanical ceiling panels of The Natural History Museum

Author

E. Charles Nelson

Subjects

Canopy, Natural history, History, Ecology, Anthropology, media_common.quotation_subject, Art, Ceiling (cloud), Agricultural and Biological Sciences (miscellaneous), Archaeology, media_common

Published

2006

184. Vapor‐Liquid Equilibria for Mixtures of Low Boiling Substances (Ternary Systems). Dechema Chemistry Data Series, Vol. VI, Part 2, 3 und 4. Von H. Knapp, S. Zeck und R. Langhorst. DECHEMA, Frankfurt/M. 1989. 3. 418 S., geb., DM 742,–.

Author

Bornhütter, K., primary

Published

1990

185. Knapp, S. Potted histories: an artistic voyage through plant exploration

Author

E. Charles Nelson

Subjects

History, Anthropology, Agricultural and Biological Sciences (miscellaneous)

Published

2004

186. Contacto con el pasado: El legado botánico de Richard Spruce

Author

León, B, Durt, T, Zappi, D, Grant, S D, Knapp, S, and BioStor

Published

2003

187. Fossil berries reveal global radiation of the nightshade family by the early Cenozoic.

Author

Deanna R, Martínez C, Manchester S, Wilf P, Campos A, Knapp S, Chiarini FE, Barboza GE, Bernardello G, Sauquet H, Dean E, Orejuela A, and Smith SD

Subjects

Fossils, Fruit, South America, Phylogeny, Capsicum, Solanum

Abstract

Fossil discoveries can transform our understanding of plant diversification over time and space. Recently described fossils in many plant families have pushed their known records farther back in time, pointing to alternative scenarios for their origin and spread. Here, we describe two new Eocene fossil berries of the nightshade family (Solanaceae) from the Esmeraldas Formation in Colombia and the Green River Formation in Colorado (USA). The placement of the fossils was assessed using clustering and parsimony analyses based on 10 discrete and five continuous characters, which were also scored in 291 extant taxa. The Colombian fossil grouped with members of the tomatillo subtribe, and the Coloradan fossil aligned with the chili pepper tribe. Along with two previously reported early Eocene fossils from the tomatillo genus, these findings indicate that Solanaceae were distributed at least from southern South America to northwestern North America by the early Eocene. Together with two other recently discovered Eocene berries, these fossils demonstrate that the diverse berry clade and, in turn, the entire nightshade family, is much older and was much more widespread in the past than previously thought., (© 2023 The Authors New Phytologist © 2023 New Phytologist Foundation.)

Published

2023

188. A new species of Oxalis (Oxalidaceae) from El Salvador

Author

Knapp, S, Sidwell, K, and BioStor

Published

2002

189. 139 Cell-specific immune-modulatory functions of S100A8/A9 in Atopic Dermatitis

Author

Irigoyen, M.P., primary, Hendrikx, T., additional, Bakiri, L., additional, Hayer, S., additional, Schaffenrath, J., additional, Starkl, P., additional, Knapp, S., additional, and Wagner, E.F., additional

Published

2023

190. H. MEUSEL; E. J. JÄGER (Hrsg.) Vergleichende Chorologie der Zentraleuropäischen Flora, Band III. Mit Beiträgen von S. BRÄUTIGAM; H.‐D. KNAPP; S. RAUSCHERT (†); E. WEINERT. Unter Mitarbeit von D. SEIDEL und J. STÖLZER und Fachwissenschaftlern aus 20 Ländern. In zwei Teilen: Textband: 333 S.; Kartenband; Karten, Literatur und Gesamtregister, 688 S., Gustav Fischer Verlag, Jena, 1992. ISBN 3‐334‐00411‐2. Preis (geb.) DM 560

Author

F. Fukarek

Subjects

media_common.quotation_subject, Plant Science, Art, Ecology, Evolution, Behavior and Systematics, media_common

Published

1994

191. Myeloid but not epithelial tissue factor exerts protective anti‐inflammatory effects in acid aspiration‐induced acute lung injury

Author

Kral‐Pointner, J.B., Schrottmaier, W.C., Horvath, V., Datler, H., Hell, L., Ay, C., Niederreiter, B., Jilma, B., Schmid, J.A., Assinger, A., Mackman, N., Knapp, S., and Schabbauer, G.

Published

2017

192. Legionella disinfection by solar concentrator system

Author

Amara, S., Baghdadli, T., Knapp, S., and Nordell, B.

Published

2017

193. High-Throughput Screening for LC3/GABARAP Binders Utilizing the Fluorescence Polarization Assay.

Author

Schwalm MP, Dopfer J, Knapp S, and Rogov VV

Subjects

Humans, Apoptosis Regulatory Proteins metabolism, Adaptor Proteins, Signal Transducing metabolism, Autophagy drug effects, Peptides metabolism, Peptides chemistry, Ligands, Autophagy-Related Protein 8 Family metabolism, Microtubule-Associated Proteins metabolism, High-Throughput Screening Assays methods, Fluorescence Polarization methods, Protein Binding

Abstract

The characterization of interactions between autophagy modifiers (Atg8-family proteins) and their natural ligands (peptides and proteins) or small molecules is important for a detailed understanding of selective autophagy mechanisms and for the design of potential Atg8 inhibitors that affect the autophagy processes in cells. The fluorescence polarization (FP) assay is a rapid, cost-effective, and robust method that provides affinity and selectivity information for small molecules and peptide ligands targeting human Atg8 proteins.This chapter introduces the basic principles of FP assays. In addition, a case study on peptide interaction with human Atg8 proteins (LC3/GABARAPs) is described. Finally, data analysis and quality control of FP assays are discussed for the proper calculation of K i values for the measured compounds., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

194. Inhibition of bromodomain and extra-terminal proteins targets constitutively active NFκB and STAT signaling in lymphoma and influences the expression of the antiapoptotic proteins BCL2A1 and c-MYC.

Author

Pieper NM, Schnell J, Bruecher D, Knapp S, and Vogler M

Subjects

Humans, Cell Line, Tumor, Gene Expression Regulation, Neoplastic drug effects, Apoptosis drug effects, Bromodomain Containing Proteins, Proteins, Minor Histocompatibility Antigens, Proto-Oncogene Proteins c-bcl-2 metabolism, Proto-Oncogene Proteins c-bcl-2 genetics, Proto-Oncogene Proteins c-myc metabolism, Proto-Oncogene Proteins c-myc genetics, Signal Transduction drug effects, NF-kappa B metabolism, Lymphoma, Large B-Cell, Diffuse metabolism, Lymphoma, Large B-Cell, Diffuse genetics, Lymphoma, Large B-Cell, Diffuse pathology

Abstract

The antiapoptotic protein BCL2A1 is highly, but very heterogeneously expressed in Diffuse Large B-cell Lymphoma (DLBCL). Particularly in the context of resistance to current therapies, BCL2A1 appears to play an important role in protecting cancer cells from the induction of cell death. Reducing BCL2A1 levels may have therapeutic potential, however, no specific inhibitor is currently available. In this study, we hypothesized that the signaling network regulated by epigenetic readers may regulate the transcription of BCL2A1 and hence that inhibition of Bromodomain and Extra-Terminal (BET) proteins may reduce BCL2A1 expression thus leading to cell death in DLBCL cell lines. We found that the mechanisms of action of acetyl-lysine competitive BET inhibitors are different from those of proteolysis targeting chimeras (PROTACs) that induce the degradation of BET proteins. Both classes of BETi reduced the expression of BCL2A1 which coincided with a marked downregulation of c-MYC. Mechanistically, BET inhibition attenuated the constitutively active canonical nuclear factor kappa-light-chain-enhancer of activated B-cells (NFκB) signaling pathway and inhibited p65 activation. Furthermore, signal transducer of activated transcription (STAT) signaling was reduced by inhibiting BET proteins, targeting another pathway that is often constitutively active in DLBCL. Both pathways were also inhibited by the IκB kinase inhibitor TPCA-1, resulting in decreased BCL2A1 and c-MYC expression. Taken together, our study highlights a novel complex regulatory network that links BET proteins to both NFκB and STAT survival signaling pathways controlling both BCL2A1 and c-MYC expression in DLBCL., (© 2024. The Author(s).)

Published

2024

195. Mast cell-derived BH4 and serotonin are critical mediators of postoperative pain.

Author

Starkl P, Jonsson G, Artner T, Turnes BL, Gail LM, Oliveira T, Jain A, Serhan N, Stejskal K, Lakovits K, Hladik A, An M, Channon KM, Kim H, Köcher T, Weninger W, Stary G, Knapp S, Klang V, Gaudenzio N, Woolf CJ, Tikoo S, Jain R, Penninger JM, and Cronin SJF

Subjects

Animals, Mice, Humans, Mice, Inbred C57BL, Substance P metabolism, Male, Mice, Knockout, Tryptophan Hydroxylase metabolism, Mast Cells immunology, Serotonin metabolism, Pain, Postoperative immunology

Abstract

Postoperative pain affects most patients after major surgery and can transition to chronic pain. The considerable side effects and limited efficacy of current treatments underline the need for new therapeutic options. We observed increased amounts of the metabolites BH4 and serotonin after skin injury. Mast cells were primary postoperative sources of Gch1 , the rate-limiting enzyme in BH4 synthesis, itself an obligate cofactor in serotonin production by tryptophan hydroxylase (Tph1). Mice deficient in mast cells or in mast cell-specific Gch1 or Tph1 showed drastically decreased postoperative pain. We found that injury induced the nociceptive neuropeptide substance P, mast cell degranulation, and granule nerve colocalization. Substance P triggered serotonin release in mouse and human mast cells, and substance P receptor blockade substantially ameliorated pain hypersensitivity. Our findings highlight the importance of mast cells at the neuroimmune interface and substance P-driven mast cell BH4 and serotonin production as a therapeutic target for postoperative pain treatment.

Published

2024

196. Discovery of Two Highly Selective Structurally Orthogonal Chemical Probes for Activin Receptor-like Kinases 1 and 2.

Author

Němec V, Remeš M, Beňovský P, Böck MC, Šranková E, Wong JF, Cros J, Williams E, Tse LH, Smil D, Ensan D, Isaac MB, Al-Awar R, Gomolková R, Ursachi VC, Fafílek B, Kahounová Z, Víchová R, Vacek O, Berger BT, Wells CI, Corona CR, Vasta JD, Robers MB, Krejci P, Souček K, Bullock AN, Knapp S, and Paruch K

Subjects

Animals, Humans, Mice, Activin Receptors, Type I antagonists & inhibitors, Activin Receptors, Type I metabolism, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors chemistry, Structure-Activity Relationship, Signal Transduction drug effects, Drug Discovery, Molecular Probes chemistry, Bone Morphogenetic Proteins metabolism, Pyrazoles chemistry, Pyrazoles pharmacology, Pyrazoles chemical synthesis, Activin Receptors, Type II metabolism, Activin Receptors, Type II antagonists & inhibitors

Abstract

Activin receptor-like kinases 1-7 (ALK1-7) regulate a complex network of SMAD-independent as well as SMAD-dependent signaling pathways. One of the widely used inhibitors for functional investigations of these processes, in particular for bone morphogenetic protein (BMP) signaling, is LDN-193189 . However, LDN-193189 has insufficient kinome-wide selectivity complicating its use in cellular target validation assays. Herein, we report the identification and comprehensive characterization of two chemically distinct highly selective inhibitors of ALK1 and ALK2, M4K2234 and MU1700 , along with their negative controls. We show that both MU1700 and M4K2234 efficiently block the BMP pathway via selective in cellulo inhibition of ALK1/2 kinases and exhibit favorable in vivo profiles in mice. MU1700 is highly brain penetrant and shows remarkably high accumulation in the brain. These high-quality orthogonal chemical probes offer the selectivity required to become widely used tools for in vitro and in vivo investigation of BMP signaling.

Published

2024

197. Targeting MYC effector functions in pancreatic cancer by inhibiting the ATPase RUVBL1/2.

Author

Vogt M, Dudvarski Stankovic N, Cruz Garcia Y, Hofstetter J, Schneider K, Kuybu F, Hauck T, Adhikari B, Hamann A, Rocca Y, Grysczyk L, Martin B, Gebhardt-Wolf A, Wiegering A, Diefenbacher M, Gasteiger G, Knapp S, Saur D, Eilers M, Rosenfeldt M, Erhard F, Vos SM, and Wolf E

Subjects

Animals, Mice, Humans, Cell Line, Tumor, Carrier Proteins metabolism, Carrier Proteins genetics, Pancreatic Neoplasms pathology, Pancreatic Neoplasms genetics, Pancreatic Neoplasms drug therapy, Pancreatic Neoplasms metabolism, ATPases Associated with Diverse Cellular Activities metabolism, ATPases Associated with Diverse Cellular Activities genetics, DNA Helicases genetics, DNA Helicases metabolism, Carcinoma, Pancreatic Ductal genetics, Carcinoma, Pancreatic Ductal pathology, Carcinoma, Pancreatic Ductal drug therapy, Carcinoma, Pancreatic Ductal metabolism, Proto-Oncogene Proteins c-myc metabolism, Proto-Oncogene Proteins c-myc genetics

Abstract

Objective: The hallmark oncogene MYC drives the progression of most tumours, but direct inhibition of MYC by a small-molecule drug has not reached clinical testing. MYC is a transcription factor that depends on several binding partners to function. We therefore explored the possibility of targeting MYC via its interactome in pancreatic ductal adenocarcinoma (PDAC)., Design: To identify the most suitable targets among all MYC binding partners, we constructed a targeted shRNA library and performed screens in cultured PDAC cells and tumours in mice., Results: Unexpectedly, many MYC binding partners were found to be important for cultured PDAC cells but dispensable in vivo. However, some were also essential for tumours in their natural environment and, among these, the ATPases RUVBL1 and RUVBL2 ranked first. Degradation of RUVBL1 by the auxin-degron system led to the arrest of cultured PDAC cells but not untransformed cells and to complete tumour regression in mice, which was preceded by immune cell infiltration. Mechanistically, RUVBL1 was required for MYC to establish oncogenic and immunoevasive gene expression identifying the RUVBL1/2 complex as a druggable vulnerability in MYC-driven cancer., Conclusion: One implication of our study is that PDAC cell dependencies are strongly influenced by the environment, so genetic screens should be performed in vitro and in vivo. Moreover, the auxin-degron system can be applied in a PDAC model, allowing target validation in living mice. Finally, by revealing the nuclear functions of the RUVBL1/2 complex, our study presents a pharmaceutical strategy to render pancreatic cancers potentially susceptible to immunotherapy., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2024. Re-use permitted under CC BY. Published by BMJ.)

Published

2024

198. Back-Pocket Optimization of 2-Aminopyrimidine-Based Macrocycles Leads to Potent EPHA2/GAK Kinase Inhibitors.

Author

Gerninghaus J, Zhubi R, Krämer A, Karim M, Tran DHN, Joerger AC, Schreiber C, Berger LM, Berger BT, Ehret TAL, Elson L, Lenz C, Saxena K, Müller S, Einav S, Knapp S, and Hanke T

Subjects

Humans, Cell Line, Tumor, Crystallography, X-Ray, Dengue Virus drug effects, Intracellular Signaling Peptides and Proteins, Macrocyclic Compounds chemistry, Macrocyclic Compounds pharmacology, Macrocyclic Compounds chemical synthesis, Models, Molecular, Protein Serine-Threonine Kinases, Structure-Activity Relationship, Morpholines, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors chemical synthesis, Pyrimidines chemistry, Pyrimidines pharmacology, Pyrimidines chemical synthesis, Receptor, EphA2 antagonists & inhibitors, Receptor, EphA2 metabolism

Abstract

Macrocyclization of acyclic compounds is a powerful strategy for improving inhibitor potency and selectivity. Here we have optimized 2-aminopyrimidine-based macrocycles to use these compounds as chemical tools for the ephrin kinase family. Starting with a promiscuous macrocyclic inhibitor, 6 , we performed a structure-guided activity relationship and selectivity study using a panel of over 100 kinases. The crystal structure of EPHA2 in complex with the developed macrocycle 23 provided a basis for further optimization by specifically targeting the back pocket, resulting in compound 55 , a potent inhibitor of EPHA2/A4 and GAK. Subsequent front-pocket derivatization resulted in an interesting in cellulo selectivity profile, favoring EPHA4 over the other ephrin receptor kinase family members. The dual EPHA2/A4 and GAK inhibitor 55 prevented dengue virus infection of Huh7 liver cells. However, further investigations are needed to determine whether this was a compound-specific effect or target-related.

Published

2024

199. Convergent evolution of plant prickles by repeated gene co-option over deep time.

Author

Satterlee JW, Alonso D, Gramazio P, Jenike KM, He J, Arrones A, Villanueva G, Plazas M, Ramakrishnan S, Benoit M, Gentile I, Hendelman A, Shohat H, Fitzgerald B, Robitaille GM, Green Y, Swartwood K, Passalacqua MJ, Gagnon E, Hilgenhof R, Huggins TD, Eizenga GC, Gur A, Rutten T, Stein N, Yao S, Poncet A, Bellot C, Frary A, Knapp S, Bendahmane M, Särkinen T, Gillis J, Van Eck J, Schatz MC, Eshed Y, Prohens J, Vilanova S, and Lippman ZB

Subjects

Evolution, Molecular, Mutation, Oryza genetics, Phylogeny, Biological Evolution, Cytokinins biosynthesis, Cytokinins genetics, Genes, Plant, Plant Epidermis anatomy & histology, Plant Epidermis genetics, Solanum anatomy & histology, Solanum genetics

Abstract

An enduring question in evolutionary biology concerns the degree to which episodes of convergent trait evolution depend on the same genetic programs, particularly over long timescales. In this work, we genetically dissected repeated origins and losses of prickles-sharp epidermal projections-that convergently evolved in numerous plant lineages. Mutations in a cytokinin hormone biosynthetic gene caused at least 16 independent losses of prickles in eggplants and wild relatives in the genus Solanum . Homologs underlie prickle formation across angiosperms that collectively diverged more than 150 million years ago, including rice and roses. By developing new Solanum genetic systems, we leveraged this discovery to eliminate prickles in a wild species and an indigenously foraged berry. Our findings implicate a shared hormone activation genetic program underlying evolutionarily widespread and recurrent instances of plant morphological innovation.

Published

2024

200. Combined Flow-Fluorescence in situ hybridization to HHV-8 and EBV reveals the viral heterogeneity of primary effusion lymphoma.

Author

Stammler R, Vacher L, Fournier B, Lemaire P, Chauvel C, Silvestrini MA, Knapp S, de Frémont GM, Meignin V, Salmona M, Legoff J, Vanjak A, Dunogué B, Urbain F, Lambotte O, Noël N, Gérard L, Oksenhendler E, Galicier L, Latour S, and Boutboul D

Subjects

Humans, Male, Aged, Middle Aged, Female, Herpesviridae Infections virology, Herpesviridae Infections diagnosis, Epstein-Barr Virus Infections virology, Epstein-Barr Virus Infections complications, Aged, 80 and over, Herpesvirus 8, Human genetics, Herpesvirus 8, Human isolation & purification, In Situ Hybridization, Fluorescence methods, Lymphoma, Primary Effusion virology, Herpesvirus 4, Human genetics, Herpesvirus 4, Human isolation & purification

Abstract

Primary effusion lymphoma (PEL) is a rare B-cell non-Hodgkin lymphoma associated with Kaposi Sarcoma-associated herpesvirus (KSHV/HHV8) infection. Lymphoma cells are coinfected with Epstein-Barr virus (EBV) in 60-80% of cases. Tools allowing a reliable PEL diagnosis are lacking. This study reports PEL diagnosis in 4 patients using a Flow-Fluorescence in situ hybridization (FlowFISH) technique that allowed detection of differentially expressed EBV and HHV8 transcripts within the same sample, revealing viral heterogeneity of the disease. Moreover, infected cells exhibited variable expressions of CD19, CD38, CD40, and CD138. Therefore, FlowFISH is a promising tool to diagnose and characterize complex viral lymphoproliferations., (© 2024 The Author(s). Journal of Medical Virology published by Wiley Periodicals LLC.)

Published

2024