Forward Genetics for Cancer Research

Dr. Jovan Mircetic
 

Forward genetics pipeline to delineate therapy resistance drivers using patient-derived organoids. © Biorender

Gastrointestinal (GI) cancers are the most frequently diagnosed malignancies and the leading cause of cancer-related deaths worldwide. The asymptotic early stages of the disease lead to most patients being diagnosed at a later stage, with large and genetically/phenotypically heterogeneous tumors. These tumors often contain multiple clones with different driver mutations that render them virtually refractive to current targeted therapies. In the case of gastric cancer (GC), for example, only two targeted therapies are available, and both offer modest benefits to the patients. The consequence of such a natural history is that all targeted therapies are currently administered with classical therapies, either chemotherapy or radiotherapy. This holds true even for new modalities, like immunotherapeutics. If, then, the current paradigm of targeted therapies (targeting driver mutations) is unlikely to be effective in highly heterogenous tumors, we propose to design new targeted therapies that will directly synergize with the classical ones and/or immunotherapy, instead of being merely orthogonal to them. For this synergy to occur, the reason for therapy failure – the development of resistance – needs to be molecularly and functionally delineated.

In our Junior Group at German Cancer Consortium (DKTK), partner site Dresden, we model the rise of the resistance to therapy in patient-derived organoids (PDOs), a physiologically relevant culture system that is shown to preserve tumor heterogeneity and can correctly predict patient responses to therapy. This modeling is done across a range of GI entities, including GC and colorectal cancer (CRC), and across a spectrum of current treatment regimens. Omics approaches are used to study genomic, transcriptomic, and proteomic changes along the evolutionary path of resistance acquisition, while functional characterization is achieved via genetic screens that utilize a range of Cas9 modalities. Taking advantage of a large organoid biobank on the campus, validations are performed directly on patient material (PDOs), and in mouse models developed by our collaborators.
 

Future projects and goals

Our main research goals lie in the identification of pathways that drive resistance to therapy and in the rational design of drugs that can resensitize resistant tumors. The focus is on resistance to chemotherapy and radiotherapy, two of the most prescribed treatment regimens for gastrointestinal cancers. By studying resistance acquisition in vitro and in vivo, we aim to identify vulnerabilities opened up by salvage pathways. In addition, we strive to pinpoint genetic markers of resistance, as patients are currently not being stratified in any way, either for chemotherapy or radiotherapy. Identifying at-risk patients and designing new synergistic therapies for them is, thus, a two-fold goal of the Mircetic laboratory.
 

Dr. Jovan Mircetic
Junior Research Group Leader - partner site Dresden

OncoRay, Technische Universität Dresden

 

 

 

Group Members

Selected Publications