Psychiatr. praxi 2017; 18(1): 7-10 | DOI: 10.36290/psy.2017.002

Research of new drugs for Alzheimer’s disease

PharmDr. Jana Hroudová, Ph.D.
Psychiatrická klinika, 1. lékařská fakulta, Univerzita Karlova a VFN v Praze, Farmakologický ústav, 1. lékařská fakulta, Univerzita Karlova a VFN v Praze, Oddělení klinické farmakologie, VFN v Praze

Alzheimer’s disease (AD) is the most common cause of dementia, however, the treatment AD options are limited and based on

administration of cholinesterase inhibitors and/or memantine, affecting glutamatergic system. Presented review article summarizes

current approaches in the research of novel agents for AD treatment; it is focused on the molecules reaching the clinical trials.

The most developed direction of pharmacotherapy is focused on pathologic β-amyloid (Aβ). Several perspective studies testing

monoclonal Aβ antibodies and β-secretase inhibitors are ongoing. Further, new cholinesterase inhibitors, monoamine oxidase

inhibitors, anti-tau immunotherapy, agents affecting serotonin and nicotine receptors, antioxidants, and others are developed.

Keywords: Alzheimer’s disease, cholinesterase inhibitors, anti-amyloid beta immunotherapy, beta secretase inhibitors, monoamine oxidase inhibitors

Published: May 1, 2017  Show citation

ACS AIP APA ASA Harvard Chicago Chicago Notes IEEE ISO690 MLA NLM Turabian Vancouver
Hroudová J. Research of new drugs for Alzheimer’s disease. Psychiatr. praxi. 2017;18(1):7-10. doi: 10.36290/psy.2017.002.
Share...
Download citation
  • BibTeX (.bib)
  • Bookends (.ris)
  • EasyBib (.ris)
  • EndNote (.enw)
  • EndNote 8 (.xml)
  • ISI WoS (.isi)
  • Medlars (.medlars)
  • Mendeley (.ris)
  • MODS (.xml)
  • Papers (.ris)
  • RefWorks (.txt)
  • RefManager (.ris)
  • RIS (.ris)
  • MS Word (.xml)
  • Zotero (.ris)
    • Open full article

    References

    1. Kapogiannis D, Mattson MP. Disrupted energy metabolism and neuronal circuit dysfunction in cognitive impairment and Alzheimer's disease. Lancet Neurol, 2011; 10(2): 187-198. Go to original source... Go to PubMed...
    2. Lipton SA. Paradigm shift in NMDA receptor antagonist drug development: molecular mechanism of uncompetitive inhibition by memantine in the treatment of Alzheimer's disease and other neurologic disorders. J Alzheimers Dis, 2004; 6(6 Suppl): S61-74. Go to original source... Go to PubMed...
    3. Soukup O, et al. A resurrection of 7-MEOTA: a comparison with tacrine. Curr Alzheimer Res, 2013; 10(8): 893-906. Go to original source... Go to PubMed...
    4. Korábečný J, et al. Synthesis and in vitro evaluation of N-(Bromobut-3-en-2-yl)-7-methoxy-1,2,3,4-tetrahydroacridin-9-amine as a cholinesterase inhibitor with regard to Alzheimer's disease treatment. Molecules, 2010; 15(12): 8804-8812. Go to original source... Go to PubMed...
    5. Zhang HY. New insights into huperzine A for the treatment of Alzheimer's disease. Acta Pharmacol Sin, 2012; 33(9): 1170-1175. Go to original source... Go to PubMed...
    6. Hroudová J, et al. Progress in drug development for Alzheimer's disease: An overview in relation to mitochondrial energy metabolism. Eur J Med Chem, 2016; 121: 774-784. Go to original source... Go to PubMed...
    7. Lu C, et al. A novel series of tacrine-selegiline hybrids with cholinesterase and monoamine oxidase inhibition activities for the treatment of Alzheimer's disease. Eur J Med Chem, 2013; 62: 745-753. Go to original source... Go to PubMed...
    8. Zhou ZD, et al. The roles of amyloid precursor protein (APP) in neurogenesis: Implications to pathogenesis and therapy of Alzheimer disease. Cell Adh Migr, 2011; 5(4): 280-292. Go to original source... Go to PubMed...
    9. Jirák, R., Nové postupy v biologické terapii demencí. Psychiatrie pro praxi, 2010; 11(4): 143-144.
    10. Tarazi H, et al. Design, synthesis and SAR analysis of potent BACE1 inhibitors: Possible lead drug candidates for Alzheimer's disease. Eur J Med Chem, 2017; 125: 1213-1224. Go to original source... Go to PubMed...
    11. Mangialasche F, et al. Alzheimer's disease: clinical trials and drug development. Lancet Neurol, 2010; 9(7): 702-716. Go to original source... Go to PubMed...
    12. Panza F, et al. Is there still any hope for amyloid-based immunotherapy for Alzheimer's disease? Curr Opin Psychiatry, 2014; 27(2): 128-137. Go to original source... Go to PubMed...
    13. Sevigny J, et al. The antibody aducanumab reduces Abeta plaques in Alzheimer's disease. Nature, 2016; 537(7618): 50-56. Go to original source... Go to PubMed...
    14. Godyn, J., et al., Therapeutic strategies for Alzheimer's disease in clinical trials. Pharmacol Rep, 2016; 68(1): 127-138. Go to original source... Go to PubMed...
    15. Vališ, M., Farmakoterapie demencí - pokroky v léčbě a aktuální doporučení. Remedia, 2013; 23(6): 396-399.
    16. Boada M, et al. Treatment of Alzheimer disease using combination therapy with plasma exchange and haemapheresis with albumin and intravenous immunoglobulin: Rationale and treatment approach of the AMBAR (Alzheimer Management By Albumin Replacement) study. Neurologia, 2016; 31(7): 473-481. Go to original source... Go to PubMed...
    17. Marcos B, et al. Signalling pathways associated with 5-HT6 receptors: relevance for cognitive effects. Int J Neuropsychopharmacol, 2010; 13(6): 775-784. Go to original source... Go to PubMed...
    18. Valasani KR, et al. Identification of human ABAD inhibitors for rescuing Abeta-mediated mitochondrial dysfunction. Curr Alzheimer Res, 2014; 11(2): 128-136. Go to original source... Go to PubMed...

    Return to the content


    Psychiatry for Practice

    Madam, Sir,
    please be aware that the website on which you intend to enter, not the general public because it contains technical information about medicines, including advertisements relating to medicinal products. This information and communication professionals are solely under §2 of the Act n.40/1995 Coll. Is active persons authorized to prescribe or supply (hereinafter expert).
    Take note that if you are not an expert, you run the risk of danger to their health or the health of other persons, if you the obtained information improperly understood or interpreted, and especially advertising which may be part of this site, or whether you used it for self-diagnosis or medical treatment, whether in relation to each other in person or in relation to others.

    I declare:

    1. that I have met the above instruction
    2. I'm an expert within the meaning of the Act n.40/1995 Coll. the regulation of advertising, as amended, and I am aware of the risks that would be a person other than the expert input to these sites exhibited

    No
    Yes

    If your statement is not true, please be aware
    that brings the risk of danger to their health or the health of others.