Inhibiteurs de PARP : leur rôle potentiel en monothérapie et en combinaison en cancer du sein triple-négatif

Beniey, Michèle

12 1900

Quatorze femmes canadiennes meurent chaque jour du cancer du sein. Le cancer du sein triple-négatif (CSTN) détient un mauvais pronostic De nombreux efforts sont fournis afin d'offrir à ces patientes des traitements ciblés, comme les inhibiteurs de poly (adenosine diphosphate-ribose) polymerase inhibitors (PARPi) afin d’améliorer leur survie et de minimiser la toxicité liée à la chimiothérapie. Le sous-groupe de CSTN qui pourrait bénéficier des PARPi reste à être identifié. De plus, différentes stratégies d'administration des PARPi et de la chimiothérapie pourraient améliorer leur efficacité thérapeutique tout en diminuant la toxicité. Nous avons précédemment dérivé une signature génétique de 63 gènes prédisant la réponse aux PARPi avec une précision globale élevée. Nos objectifs sont 1) d'évaluer les implications cliniques de la signature génétique; et 2) de déterminer la séquence optimale d'administration du talazoparib et du carboplatin in vivo en cancer du sein triple-négatif BRCAWT. D'abord, nous avons évalué la fréquence mutationnelle des 63 gènes dans différents contextes cliniques. Deux bases de données publiques furent utilisées. Puis, nous avons comparé trois cohortes de xénogreffes orthotopiques: A) talazoparib en premier, combiné au carboplatin le jour 3; carboplatin en premier suivi du talazoparib B) un jour après; et C) sept jours après. La fréquence mutationnelle des 63 gènes était élevée chez les tumeurs luminales B et celles de mauvais pronostic. Les patientes luminales B mutées avaient une moindre survie que les patientes non mutées. Aussi, l'inhibition tumorale et métastatique était similaire pour les cohortes A et B, cependant la cohorte B avait moins de toxicité. Les PARPi pourraient avoir un rôle chez les tumeurs luminales B et celles de mauvais pronostic. Deuxièmement, le prétraitement avec le carboplatin semble améliorer la sensibilité au talazoparib et diminuer la toxicité. / Fourteen Canadian women die every day from breast cancer. Triple-negative breast cancer (TNBC) has a poor prognosis. Numerous efforts are made to offer these patients targeted therapies such as poly (adenosine diphosphate-ribose) polymerase inhibitors (PARPi) to improve survival and minimize chemotherapy-related toxicity. It is not well understood which subset of TNBC patients will benefit from PARPi; and if different sequencing strategies of PARPi and chemotherapy can improve therapeutic efficacy and decrease toxicity. We previously derived a 63-gene signature predicting response to PARPi with a high overall accuracy. Our objectives are 1) to evaluate the clinical implications of the 63-gene signature; and 2) to determine the optimal sequence of administration of talazoparib and carboplatin in vivo in BRCAWT TNBC. First, we evaluated the mutational frequency of the 63 genes in different clinical settings using two publically-available datatsets. Second, we compared three cohorts of orthotopic xenografts: A) talazoparib first, combined with carboplatin on day 3; carboplatin first, followed by talazoparib B) one day later; and C) seven days later. We found that the mutational frequency was high in breast cancer subtypes of poor prognosis. Mutated luminal B patients had a lower survival than non-mutated patients. We also found that tumoral and metastatic inhibition were similar between cohorts A and B, but cohort B had less toxicity. In conclusion, there is potential for PARPi efficacy in luminal B and poor prognosis tumors. Second, pretreatment with carboplatin may be an effective approach with less toxicity.

signature génétique

cancer du sein

cancer du sein triple-négatif

chimiothérapie

thérapie ciblée

inhibiteurs de PARP

xénogreffe orthotopique

métastases

toxicité

combinaison de traitement

Gene signature

Breast cancer

Triple-negative breast cancer

Chemotherapy

Targeted therapy

PARP inhibitors

Orthotopic xenograft

Metastasis

Toxicity

Combination treatment

Weighted gene co-expression network analysis of colorectal patients to identify right drug-right target for potent efficacy of targeted therapy

Tripathi, Anamika

10 December 2017

Indiana University-Purdue University Indianapolis (IUPUI) / Colon rectal cancer (CRC) is one of the most common cancers worldwide. It is characterized by the successive accumulation of mutations in genes controlling epithelial cell growth and differentiation leading to genomic in-stability. This results in the activation of proto-oncogene(K-ras), loss of tumor suppressor gene activity and ab-normality in DNA repair genes. Targeted therapy is a new generation of cancer treatment in which drugs attack targets which are specific for the cancer cell and are critical for its survival or for its malignant behavior. Survival of metastatic CRC patients has approximately doubled due to the development of new combinations of stan-dard chemotherapy, and the innovative targeted therapies, such as monoclonal antibodies against epidermal growth factor receptor (EGFR) or monoclonal antibodies against vascular endothelial growth factor (VEGFR).The study is to exhibit the need for right drug-right target and provides a proof of principle for potent efficacy of molecular targeted therapy for CRC. We have performed the weighted gene co-expression network analysis for three different patient cohort treated with different targeted therapy drugs. The results demonstrates the variation across different treatment regime in context of transcription factor networks. New significant tran-scription factors have been identified as potential biomarker for CRC cancer including EP300, STAT6, ATF3, ELK1, HNF4A, JUN, TAF1, IRF1, TP53, ELF1 and YY1. The results provides guidance for future omic study on CRC and additional validation work for potent biomarker for CRC.

Colorectal Cancer(CRC)

molecular targeted therapy

co-expression network

cetuximab treated patient

weighted gene co-expression

differentially expressed gene

co-expression module

module preservation

patient cohort

pathway analysis

epidermal growth factor receptor

vascular endothelial growth factor

transcription factor

transcriptional mi regulation

gene expression

chemotherapy

Established and Emerging Treatments of Skin GvHD

Link-Rachner, Cornelia S., Sockel, Katja, Schuetz, Catharina

30 May 2024

Graft-versus-host disease (GvHD) of the skin is a severe allo-immune reaction and complication following allogeneic stem cell transplantation. Over the past years, intensive pre-clinical research has led to an improved understanding of the pathophysiology of acute and to a lesser extend chronic GvHD. This has translated into the approval of several new agents for the treatment of both forms of GvHD. This review summarizes the most recent advances in underlying pathomechanisms, clinical trials and newly approved agents for GvHD, with a special focus on skin involvement.

info:eu-repo/classification/ddc/610

ddc:610

Reversing Cancer Cell Fate: Driving Therapeutic Differentiation of Hepatoblastoma to Functional Hepatocyte-Like Cells

Smith, Jordan L.

20 March 2020

Background & Aims: Despite advances in surgical care and chemotherapeutic regimens, the five-year survival rate for Stage IV Hepatoblastoma (HB), the predominant pediatric liver tumor, remains at 27%. YAP1 and β-Catenin co-activation occurs in 80% of children’s HB; however, a lack of conditional genetic models precludes exploration of tumor maintenance and therapeutic targets. Thus, the clinical need for a targeted therapy remains unmet. Given the predominance of YAP1 and β-catenin activation in children’s tumors, I sought to evaluate YAP1 as a therapeutic target in HB. Approach & Results: Herein, I engineered the first conditional murine model of HB using hydrodynamic injection to deliver transposon plasmids encoding inducible YAP1S127A, constitutive β-CateninDelN90, and a luciferase reporter to murine liver. Tumor regression was evaluated using in vivo bioluminescent imaging, and tumor landscape characterized using RNA sequencing, ATAC sequencing and DNA foot-printing. Here I show that YAP1 withdrawal in mice mediates >90% tumor regression with survival for 230+ days. Mechanistically, YAP1 withdrawal promotes apoptosis in a subset of tumor cells and in remaining cells induces a cell fate switch driving therapeutic differentiation of HB tumors into Ki-67 negative “hbHep cells.” hbHep cells have hepatocyte-like morphology and partially restored mature hepatocyte gene expression. YAP1 withdrawal drives formation of hbHeps by modulating liver differentiation transcription factor (TF) occupancy. Indeed, tumor-derived hbHeps, consistent with their reprogrammed transcriptional landscape, regain partial hepatocyte function and can rescue liver damage in mice. Conclusions: YAP1 withdrawal, without modulation of oncogenic β-Catenin, significantly regresses hepatoblastoma, providing the first in vivo data to support YAP1 as a therapeutic target for HB. Modulating YAP1 expression alone is sufficient to drive long-term regression in hepatoblastoma because it promotes cell death in a subset of tumor cells and modulates transcription factor occupancy to reverse the fate of residual tumor cells to mimic functional hepatocytes.

Therapeutic Differentiation

Targeted Therapy

Pediatric Cancer

Oncogene

Liver cancer

Mouse Model

Conditional Model

Genetic

Inducible

Hepatoblastoma

Oncogene Addiction

Tumor Dormancy

Drug Discovery

YAP

B-Catenin

Hydrodynamic Injection

Sleeping Beauty System

Tranposase

Lineage Tracing

Cancer Biology

Cell Biology

Digestive System

Digestive System Diseases

Disease Modeling

Gastroenterology

Genetic Processes

Genetics

Hepatology

Laboratory and Basic Science Research

Medical Molecular Biology

Molecular Genetics

Neoplasms

Oncology

Pediatrics

Translational Medical Research