Lessons learned from protein aggregation: toward technological and biomedical applications

César L Avila; Silvina Chaves; Sergio B Socias; Esteban Vera-Pingitore; Florencia González-Lizárraga; Cecilia Vera; Diego Ploper; Rosana Chehín

doi:10.1007/s12551-017-0317-z

Lessons learned from protein aggregation: toward technological and biomedical applications

Biophys Rev. 2017 Oct;9(5):501-515. doi: 10.1007/s12551-017-0317-z. Epub 2017 Sep 13.

Authors

César L Avila^{1

2}, Silvina Chaves^{1

2}, Sergio B Socias^{1

2}, Esteban Vera-Pingitore^{1

2}, Florencia González-Lizárraga^{1

2}, Cecilia Vera^{1

2}, Diego Ploper^{1

2}, Rosana Chehín^{3

4}

Affiliations

¹ Instituto Superior de Investigaciones Biológicas (INSIBIO), Centro Científico Tecnológico (CCT) Tucumán, CONICET-Universidad Nacional de Tucumán (CONICET-UNT), Crisóstomo Alvarez 722, Tucumán, Argentina.
² Instituto de Química Biológica Dr. Bernabé Bloj, Facultad de Bioquímica, Química y Farmacia, Universidad Nacional de Tucumán, Chacabuco 461, Tucumán, T4000ILI, Argentina.
³ Instituto Superior de Investigaciones Biológicas (INSIBIO), Centro Científico Tecnológico (CCT) Tucumán, CONICET-Universidad Nacional de Tucumán (CONICET-UNT), Crisóstomo Alvarez 722, Tucumán, Argentina. rosana@fbqf.unt.edu.ar.
⁴ Instituto de Química Biológica Dr. Bernabé Bloj, Facultad de Bioquímica, Química y Farmacia, Universidad Nacional de Tucumán, Chacabuco 461, Tucumán, T4000ILI, Argentina. rosana@fbqf.unt.edu.ar.

Abstract

The close relationship between protein aggregation and neurodegenerative diseases has been the driving force behind the renewed interest in a field where biophysics, neurobiology and nanotechnology converge in the study of the aggregate state. On one hand, knowledge of the molecular principles that govern the processes of protein aggregation has a direct impact on the design of new drugs for high-incidence pathologies that currently can only be treated palliatively. On the other hand, exploiting the benefits of protein aggregation in the design of new nanomaterials could have a strong impact on biotechnology. Here we review the contributions of our research group on novel neuroprotective strategies developed using a purely biophysical approach. First, we examine how doxycycline, a well-known and innocuous antibiotic, can reshape α-synuclein oligomers into non-toxic high-molecular-weight species with decreased ability to destabilize biological membranes, affect cell viability and form additional toxic species. This mechanism can be exploited to diminish the toxicity of α-synuclein oligomers in Parkinson's disease. Second, we discuss a novel function in proteostasis for extracellular glyceraldehyde 3-phosphate dehydrogenase (GAPDH) in combination with a specific glycosaminoglycan (GAG) present in the extracellular matrix. GAPDH, by changing its quaternary structure from a tetramer to protofibrillar assembly, can kidnap toxic species of α-synuclein, and thereby interfere with the spreading of the disease. Finally, we review a brighter side of protein aggregation, that of exploiting the physicochemical advantages of amyloid aggregates as nanomaterials. For this, we designed a new generation of insoluble biocatalysts based on the binding of photo-immobilized enzymes onto hybrid protein:GAG amyloid nanofibrils. These new nanomaterials can be easily functionalized by attaching different enzymes through dityrosine covalent bonds.

Keywords: Alzheimer’s disease; Amyloid; Amyloid functionalization; Cross-beta structure; Glycosaminoglycan; Parkinson’s disease; Protein aggregation.

Publication types

Review