Abstract
Background: The oxidation of methionine residue in position 35 of Ab to sulphoxide (Ab-sulphoxide) has the ability to deeply modify wild-type Ab 1â42 (Ab) neurotoxic action. Our previous studies suggest that in nucleated cells, lower toxicity of Ab-sulphoxide might result not from structural alteration, but from elevation of methionine sulphoxide reductase A (MsrA) activity and mRNA levels. Design: On this basis, we hypothesised that red blood cell (RBC), a cell devoid almost completely of MsrA activity, shares with nucleated cells an antioxidant system induced by methionine 35 sulphoxide, responsible for the lower toxicity of Ab-sulphoxide in RBC. (Results) Supporting this hypothesis, we found that the low toxicity of Ab-sulphoxide in RBC correlated with pentose phosphate pathway (PPP) flux increase, and this event was associated with a low level of methionine oxidation in total proteins. None of these effects were observed when cells were exposed to Ab native. Discussion: These results outline the importance of the redox state of methionine 35 in the modulation of Ab-mediated events and suggest an important protective role for PPP in RBC of patients affected by Alzheimer's disease.
| Lingua originale | English |
|---|---|
| pagine (da-a) | 314-321 |
| Numero di pagine | 8 |
| Rivista | European Journal of Clinical Investigation |
| Volume | 47 |
| DOI | |
| Stato di pubblicazione | Pubblicato - 2017 |
Keywords
- Alzheimer Disease
- Alzheimer's disease
- Amyloid beta-Peptides
- Antioxidants
- Biochemistry
- Caspase 3
- Clinical Biochemistry
- Erythrocytes
- Glucose
- Healthy Volunteers
- Humans
- Methionine
- Methionine Sulfoxide Reductases
- Oxidation-Reduction
- Pentose Phosphate Pathway
- amyloid beta-peptide (1â42)
- caspase 3
- methionine 35
- oxidative stress
- pentose phosphate pathway
- red blood cell