Literature DB >> 19689341

Fcgamma receptor 1 (CD64), a target beyond cancer.

T Thepen1, M Huhn, G Melmer, M K Tur, S Barth.   

Abstract

Immunotoxins are powerful tools to specifically eliminate deviated cells. Due to the side effects of the original immunotoxins, they were only considered for the treatment of cancer as in these cases, the potential favourable effect outweighed the unwanted toxic side effects. Over time, many improvements in the construction of immunotoxins have been implemented that circumvent, or at least strongly diminish, the side effects. In consequence this opens the way to employ these immunotoxins for the treatment of non-life threatening diseases. One such category of disease could be the many chronic inflammatory disorders in which an uncontrolled interaction between inflammatory cells leads to chronicity. In several of these chronic conditions, activated macrophages, which are characterised by an increased expression of CD64, are known to play a key role. In this review we discuss the data presently available on elimination of activated macrophages through CD64 immunotoxins in several animal models for chronic disease. A chemically linked complete antibody with the plant toxin Ricin-A, proved very effective and provided proof of concept. Subsequently, the development towards genetically engineered, fully human, multivalent single chain based immunotoxins that have diminished immunogenicity, is discussed. The data show that the specific elimination of activated macrophages through CD64 is indeed beneficial for the course of disease. As opposed to other methods used to inactivate or eliminate macrophages, with the CD64 based immunotoxins only the activated population is killed. This may open the way to apply these immunotoxins as therapeutics in chronic inflammatory disease.

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Year:  2009        PMID: 19689341     DOI: 10.2174/138161209788923967

Source DB:  PubMed          Journal:  Curr Pharm Des        ISSN: 1381-6128            Impact factor:   3.116


  8 in total

Review 1.  Evolution of the magic bullet: Single chain antibody fragments for the targeted delivery of immunomodulatory proteins.

Authors:  Christian Fercher; Sahar Keshvari; Michael A McGuckin; Ross T Barnard
Journal:  Exp Biol Med (Maywood)       Date:  2017-12-19

2.  Monomeric IgG1 Fc molecules displaying unique Fc receptor interactions that are exploitable to treat inflammation-mediated diseases.

Authors:  Tianlei Ying; Yang Feng; Yanping Wang; Weizao Chen; Dimiter S Dimitrov
Journal:  MAbs       Date:  2014       Impact factor: 5.857

3.  Optimal structural design of mannosylated nanocarriers for macrophage targeting.

Authors:  Peiming Chen; Xiaoping Zhang; Lee Jia; Robert K Prud'homme; Zoltan Szekely; Patrick J Sinko
Journal:  J Control Release       Date:  2014-09-16       Impact factor: 9.776

Review 4.  Fc Engineering for Developing Therapeutic Bispecific Antibodies and Novel Scaffolds.

Authors:  Hongyan Liu; Abhishek Saxena; Sachdev S Sidhu; Donghui Wu
Journal:  Front Immunol       Date:  2017-01-26       Impact factor: 7.561

5.  FCGR1A Serves as a Novel Biomarker and Correlates With Immune Infiltration in Four Cancer Types.

Authors:  Ji-Li Xu; Yong Guo
Journal:  Front Mol Biosci       Date:  2020-12-03

6.  Artificial Neural Network-Based Study Predicts GS-441524 as a Potential Inhibitor of SARS-CoV-2 Activator Protein Furin: a Polypharmacology Approach.

Authors:  M Dhanalakshmi; Kajari Das; Medha Pandya; Sejal Shah; Ayushman Gadnayak; Sushma Dave; Jayashankar Das
Journal:  Appl Biochem Biotechnol       Date:  2022-10       Impact factor: 3.094

7.  Neutrophils in chronic lymphocytic leukemia are permanently activated and have functional defects.

Authors:  Gayane Manukyan; Tomas Papajik; Petr Gajdos; Zuzana Mikulkova; Renata Urbanova; Gabriela Gabcova; Milos Kudelka; Peter Turcsányi; Pavlina Ryznerova; Vit Prochazka; Eva Kriegova
Journal:  Oncotarget       Date:  2017-08-08

Review 8.  CD64: An Attractive Immunotherapeutic Target for M1-type Macrophage Mediated Chronic Inflammatory Diseases.

Authors:  Olusiji A Akinrinmade; Shivan Chetty; Adebukola K Daramola; Mukit-Ul Islam; Theo Thepen; Stefan Barth
Journal:  Biomedicines       Date:  2017-09-12
  8 in total

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