Biomarkers in Alzheimer's Disease Analysis by Mass Spectometry- Based Proteomics

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Mindmap am Biomarkers in Alzheimer's Disease Analysis by Mass Spectometry- Based Proteomics, erstellt von María A am 02/11/2017.
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María A
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Zusammenfassung der Ressource

Biomarkers in Alzheimer's Disease Analysis by Mass Spectometry- Based Proteomics
  1. BIOMARKER: substance used as measurable indicator of a particular biological state (normal or pathologic)
    1. IT SHOULD REFLECT: progression of disease providing better prognosis and early diagnosis
      1. based on mass specrometry proteomics (whose goal is to identify and quantify proteins from biological samples)
        1. SOURCES: human samples (fluids: blood, CSF, urine and saliva. DNA (and modifications), RNA, miRNA, proteins (PTM)
      2. 3 PHASES IN THE DEVELOPMENT OF A NEW ONE
        1. DISCOVERY PHASE: proteomic techniques are applied to blood or CSF to identify candidates
          1. VERIFICATION PHASE: quantify the candidates to confirm differential expression in blood/CSF from cases vs controls
            1. VALIDATION PHASE: considered for further clinical evaluation
              1. MRM-MS and immunoassay
              2. MRM-LC-MS/MS
              3. LC-MS/MS with fractionation
            2. TYPES
              1. DNA- BASED
                1. BLOOD- BASED:
                  1. CSF- BASED
                    1. PROTEINS: 0.15-0.45 g/L in plasma, proximal to the CNS (interacts with brain, reflects its biochemical changes), highly invasive, contáis components form the blood and CNS
                      1. MS, microarray, 2D gel
                        1. changes at protein levels are associated with AD
                          1. basic biomarker: albumin (biomarker for blood brain barrier BBB)
                            1. increase= BBB damage
                            2. sPLA2 is a BBB factor
                              1. increase= BBB damage
                              2. Visinin-like 1 increased after stroke
                                1. increase in tau/pTau= MCI to AD
                                  1. increase in neurofilament proteins= neuronal damage
                                    1. downgrade in FAB3, CHGA, B, Neurogranin
                                      1. elevated S-100B, GFAP
                                        1. related to Aβ
                                          1. BACE1, sAPPα/sAPPβ, or Aβ oligomers
                                  2. PROTEINS: 60-80 g/L in plasma, blood is in contact with all cells, easily accesible (non-invasive), cost-time efficient, can be separated into components (plasma and serum)
                                    1. MS, microarray, 2D gel
                                      1. changes at protein levels are associated with AD
                                        1. downregulated Aβ (plasma biomarker)
                                          1. upregulated ApoE (chromosome 19)
                                            1. IL-1α, IL-6 (increase risk)
                                              1. Clusterin: ilipoprotein that is part of amyloid plaques
                                                1. increased α-1-antichymotrypsin: inflammatory cascade and formation od amyloid fibrils
                                                  1. downregulated ADNP in early phase
                                            2. DNA methylation studies. Obtained from cells and exosomes in plasma
                                              1. miRNA: non-coding, players of postranscriptional gene modification
                                                1. DETECTED BY: RT-PCR, microarray and sequencing, 2D gel
                                                  1. changes at miRNA levels are associated with AD
                                                    1. upregulation: miR-9,-125,-128, -34a, -145b, -155
                                                      1. downregulation: miR-107, -137, -181c, -9, -29b, -146a
                                              2. PROTEOMIC TECNIQUES
                                                1. they include several components: sample preparation, primary separation, protein or peptide identification and bioinformatic data analysis.
                                                  1. 2D GEL
                                                    1. LC-mass spectometry
                                                      1. clinical testing
                                                        1. radioimmunoassays
                                                          1. Western-blott
                                                            1. ELISA
                                                              1. MRM-Mass spectrometry
                                                          2. ALZHEIMER'S DISEASE (AD) develops slowly from 1) preclinical phase to 2) clinical syndrome
                                                            1. BIOMARKERS CURRENLY USED: primary (Aβ and tau)
                                                              1. possible biomarkers
                                                              2. TAREA 09 ARRIOLA VÁZQUEZ MARÍA JOSÉ, GARCÍA ECHEVERRIA GALA, JIMENEZ DELGADO ZOHE MUÑOZ-LEDO CERON PAULINA,
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