Das CeMM - Forschungszentrum für Molekulare Medizin GmbH - Drug pipelines, Patents, Clinical trials

Overview

Tags

Neoplasms

Immune System Diseases

Hemic and Lymphatic Diseases

Proteolysis-targeting chimeras (PROTAC)

Small molecule drug

CRISPR/Cas9

Disease domain score

A glimpse into the focused therapeutic areas

Technology Platform

Most used technologies in drug development

Targets

Most frequently developed targets

Disease Domain	Count

Neoplasms	6
Immune System Diseases	2
Hemic and Lymphatic Diseases	1

Top 5 Drug Type	Count

Proteolysis-targeting chimeras (PROTAC)	5
Small molecule drug	3
Chemical drugs	1
CRISPR/Cas9	1

Top 5 Target	Count

NHE1(Sodium/hydrogen exchanger 1)	4
DDB1 x SLC29A1	2
BET(Bromodomain and extra terminal domain protein)	1
RHOG(ras homolog family member G)	1
TASL(TLR adaptor interacting with endolysosomal SLC15A4)	1

The humanSLC39A8(hSLC39A8) gene encodes a plasma membrane protein SLC39A8 (ZIP8) that mediates the specific uptake of the metals Cd2+, Mn2+, Zn2+, Fe2+, Co2+, and Se4+. Pathogenic variants withinhSLC39A8are associated with congenital disorder of glycosylation type 2 (CDG type II) or Leigh-like syndrome. However, numerous mutations of uncertain significance are also linked to different conditions or benign traits. Our study characterized 21hSLC39A8variants and measured their impact on protein localization and intracellular levels of Cd2+, Zn2+, and Mn2+. We identified four variants that disrupt protein expression, five variants with high retention in the endoplasmic reticulum, and 12 variants with localization to the plasma membrane. From the 12 variants with plasma membrane localization, we identified three with complete loss of detectable ion uptake by the cell and five with differential uptake between metal ions. Further in silico analysis on protein stability identified variants that may affect the stability of homodimer interfaces. This study elucidates the variety of effects ofhSLC39A8variants on ZIP8 and on diseases involving disrupted metal ion homeostasis.

01 Jul 2024·LEUKEMIA

The gray area of RQ-PCR-based measurable residual disease: subdividing the “positive, below quantitative range” category

Article

Author: Pott, Christiane ; Clappier, Emmanuelle ; Drandi, Daniela ; van der Velden, Vincent H J ; Schilhabel, Anke ; Cazzaniga, Gianni ; Kotrova, Michaela ; Trka, Jan ; Hancock, Jeremy ; van Dongen, Jacques J M ; Ritgen, Matthias ; Hoogeveen, Patricia ; Eckert, Cornelia ; Fronkova, Eva ; Brüggemann, Monika ; Svaton, Michael ; Schäfer, Beat W ; Schön, Felix ; Skotnicova, Aneta

01 Jun 2024·Nature chemistry

Deciphering functional roles of protein succinylation and glutarylation using genetic code expansion

Article

Author: Lang, Kathrin ; Weyh, Maria ; Nguyen, Tuan-Anh ; Fottner, Maximilian ; Jokisch, Marie-Lena

Abstract:

Post-translational modifications (PTMs) dynamically regulate cellular processes. Lysine undergoes a range of acylations, including malonylation, succinylation (SucK) and glutarylation (GluK). These PTMs increase the size of the lysine side chain and reverse its charge from +1 to −1 under physiological conditions, probably impacting protein structure and function. To understand the functional roles of these PTMs, homogeneously modified proteins are required for biochemical studies. While the site-specific encoding of PTMs and their mimics via genetic code expansion has facilitated the characterization of the functional roles of many PTMs, negatively charged lysine acylations have defied this approach. Here we describe site-specific incorporation of SucK and GluK into proteins via temporarily masking their negative charge through thioester derivatives. We prepare succinylated and glutarylated bacterial and mammalian target proteins, including non-refoldable multidomain proteins. This allows us to study how succinylation and glutarylation impact enzymatic activity of metabolic enzymes and regulate protein–DNA and protein–protein interactions in biological processes from replication to ubiquitin signalling.

1

News (Medical) associated with Das CeMM - Forschungszentrum für Molekulare Medizin GmbH

28 Sep 2022

·www.sciencedaily.com

Study demonstrates that ticks weaken skin's immune response

Hitherto, scientists have not fully understood why ticks are such dangerous disease vectors. A research team now shows that tick saliva inhibits the skin's defense function, thereby increasing the risk of diseases such as tick-borne encephalitis (TBE) or Lyme disease. Hitherto, scientists have not fully understood why ticks are such dangerous disease vectors. A research team led by Johanna Strobl and Georg Stary from MedUni Vienna's Department of Dermatology shows that tick saliva inhibits the skin's defence function, thereby increasing the risk of diseases such as tick-borne encephalitis (TBE) or Lyme disease. The study was recently published in the Journal of Clinical Investigation. The researchers carried out their investigations on skin samples from volunteers and also on models of human skin, mimicking the bite of the most common European tick (Ixodes ricinus). In both cases, the team led by Georg Stary (MedUni Vienna's Department of Dermatology, CeMM Research Center for Molecular Medicine of the Austrian Academy of Sciences, Ludwig Boltzmann Institute for Rare and Undiagnosed Diseases) in collaboration with the research group of Hannes Stockinger (Center for Pathophysiology, Infectiology and Immunology at MedUni Vienna) identified rapidly occurring patterns of immunomodulation. For example, it was found that the function of immune cells, especially T cells, which are important for immunological memory, was disrupted by contact with tick saliva. Tick saliva modulates immune system The scientists made similar observations in early stages of model infection by Borrelia burgdorferi, the most common cause of Lyme disease. They found that pre-incubation of Lyme disease-transmitting bacteria (B. burgdorferi spirochetes) with tick salivary gland extracts impedes the accumulation of immune cells in the skin and increases the pathogen burden. "Overall, we found that tick feeding causes profound changes in the skin's immune system inhibiting the local immune response. This means that dangerous pathogens that are introduced into the skin together with tick saliva, can multiply more easily, leading to infection," says Johanna Strobl, lead author of the study, summarising the main research findings. Climate change increases danger from ticks Austria is one of the countries with the greatest prevalence of ticks. Nearly every second European tick is infected with pathogens, Lyme disease and tick-borne encephalitis (TBE) being the most common tick-borne diseases. The arachnids become active at a temperature of seven degrees. Due to rising temperatures associated with climate change, ticks now also pose a threat in higher-altitude regions of Austria and well into late autumn.

100 Deals associated with Das CeMM - Forschungszentrum für Molekulare Medizin GmbH

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100 Translational Medicine associated with Das CeMM - Forschungszentrum für Molekulare Medizin GmbH

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Pipeline

Pipeline Snapshot as of 19 Mar 2025

The statistics for drugs in the Pipeline is the current organization and its subsidiaries are counted as organizations,Early Phase 1 is incorporated into Phase 1, Phase 1/2 is incorporated into phase 2, and phase 2/3 is incorporated into phase 3

Discovery

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8

Preclinical

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Current Projects

Drug(Targets)	Indications	Global Highest Phase

d9A-5 ( NHE1 )	Neoplasms More	Preclinical
d9A-4 ( NHE1 )	Neoplasms More	Preclinical
d9A-3 ( NHE1 )	Neoplasms More	Preclinical
Feeblin ( TASL )	Systemic Lupus Erythematosus More	Preclinical
d9A-1 ( NHE1 )	Neoplasms More	Preclinical