Life Science and Technology News
Sensitivity-enhanced solid-state NMR spectroscopy can be used in the structural characterization of amyloid β—the pathogenic protein involved in Alzheimer's disease—as shown by scientists from Tokyo Tech. Their findings bring to light a novel polymorph of the protein and associated structural elements that can be targeted for disruption towards development of new AD treatment strategies.
Alzheimer's disease (AD) is a neurological condition leading to dementia that worsens with age as patients exhibit cognitive, memory, and psychological deficits. While current therapies focus on relieving these symptoms to some extent, AD does not have a definite prevention or cure, suggesting the need for continued efforts towards understanding the biology of the disease.
Accumulation of the pathogenic amyloid β (Aβ) protein fibrils in the form of plaques in the brain is a hallmark of AD. Deciphering its structural organization is thus crucial for designing targeted treatments against the disease. While several different forms, or polymorphs, of Aβ40 species of the protein have been reported, less is understood about the more pathogenic species, Aβ42. Moreover, characterizing trace amounts of Aβ from small sample amount using standard analytical techniques still remains a challenge.
Thus, a team of researchers from Tokyo Institute of Technology, RIKEN, University of Illinois at Chicago, and University of Chicago, led by Prof. Yoshitaka Ishii, have tested the applicability of solid-state nuclear magnetic resonance (SSNMR) spectroscopy in deciphering the atomic level structural differences of Aβ and associated pathogenic fibrils. Their findings are published in the Journal of the American Chemical Society. This powerful analytical technique measures differential behavior and properties of nuclei under the influence of magnetic and electric fields, highlighting their atomic structure.
Giving a further insight into their study, Prof. Ishii states, "Limited information is available on structural variations of Aβ42 fibrils prepared at physiologically relevant conditions, despite their pathological importance. In our study, we demonstrate the use of 1H (hydrogen isotope)-detected SSNMR in the characterization of patient derived, as well as synthetic Aβ fibrils in limited amounts as low as pico- to nano-moles."
13C (carbon isotope)-detected SSNMR, traditionally used for structural characterization, requires large sample amounts and poses difficulties in the preparation of homogenous samples. Given the higher sensitivity and ease of analyzing trace amounts in biological samples, the researchers have used sensitivity enhanced 1H detected SSNMR for their analysis. Synthetic fibrils and brain derived Aβ from a patient with Alzheimer's disease were labeled with isotopes 13C and 15N at specific amino acid residues for enhanced sensitivity, atomic resolution, and site-specific structural analysis.
The team was able to successfully characterize a novel polymorph of Aβ42 using the aforementioned approach, with only about 42 nmol of Aβ—25 to 100 times less than previously used amount. Furthermore, sensitivity enhancement significantly decreased the time required to obtain the spectra of the samples. Spectral positions obtained by this technique revealed that the structure of the protein backbone as well as the arrangement of the side chains are distinct from structures previously reported.
Overall, the study elucidates the molecular contacts involved in stabilizing pathogenic Aβ42 fibrils, thus paving way for novel therapeutic strategies that can target these toxic aggregates that drive AD progression.
Prof. Ishii concludes stating the clinical applications of their findings, "Our study demonstrates the propensity of Aβ42 to form multiple forms of fibrils, in the brain as well as in synthetic preparations. We believe that our study can open new avenues for analyzing trace amounts of biological samples such as amyloid fibrils and oligomers, for which 13C-detected SSNMR might be ineffective."
We are a step closer towards understanding this complex disease indeed!
This project was supported by the JST-Mirai Program (grant no. JPMJMI17A2, Japan), NIH grants (U01 grant 5U01GM098033; R01AG048793), JSPS KAKENHI grant (no. JP15K21772, Japan), Alzheimer's Association Zenith Fellowship Award, and the Medical Scientist Training Program grant (no: T32 GM07281).
|Authors :||Ayesha Wickramasinghe,1, 2 Yiling Xiao,4 Naohiro Kobayashi,2, 3 Songlin Wang,4 Kathryn P. Scherpelz,5 Toshio Yamazaki,2,3 Stephen C. Meredith,5, 6 Yoshitaka Ishii1, 2, 3, 4*|
|Title of original paper :||Sensitivity-Enhanced Solid-state NMR Detection of Structural Differences and Unique Polymorphs in Pico- to Nanomolar Amounts of Brain-derived and Synthetic 42-residue Amyloid-β Fibrils|
|Journal :||Journal of the American Chemical Society|
1 School of Life Science and Technology, Tokyo Institute of Technology, Japan
2 NMR Division, RIKEN, Japan
3 RIKEN Center for Biosystems Dynamics Research, Japan
4 Department of Chemistry, University of Illinois at Chicago, USA
5 Department of Biochemistry and Molecular Biology, University of Chicago, USA
6 Department of Pathology, University of Chicago, USA
|* Corresponding author’s email:||firstname.lastname@example.org|
School of Life Science and Technology
—Unravel the Complex and Diverse Phenomena of Life—
Information on School of Life Science and Technology inaugurated in April 2016