TY  - BOOK
AU  - Muhammad Muneeb Muhammad Abdulazeem,
AU  - Dalaal Moustafa Abdallah  
AU  - Hanan Salah El-Din El-Abhar
AU  - Walaa Wadie Ibrahim 
AU  - Yasmin Saad Abulfadl
TI  - Potential mechanisms of ticagrelor in modulating  neurodegeneration in rotenone-induced parkinsonism in rats
U1  - 615.1 
PY  - 2025///
KW  - Drugs
KW  - Ø§ÙØ¹ÙØ§ÙÙØ±
KW  - Ticagrelor
KW  - Rotenone
KW  - Parkinson's disease
KW  - Endoplasmic-reticulum stress
KW  - Apoptosis
KW  - Autophagy
N1  - Thesis (Ph.D)-Cairo University, 2025; Bibliography: pages 78-107.; Issues also as CD
N2  - 	Cardiovascular diseases, such as myocardial infarction, ischemic stroke, and coronary heart ailments have been closely associated with Parkinsonâs disease (PD). Despite this established link, the potential neuroprotective impact of the potent antiplatelet agent ticagrelor (Tica) remains unexplored against PD. Thus, we hypothesized that Tica could be repurposed as a therapeutic agent against PD. 
	The rotenone experimental model was adopted in Wistar male rats by administering rotenone subcutaneously on alternate days during a 21-day experimental period and treating a subset of rats with Tica orally for the last 11 consecutive days.
	The administration of Tica improved motor function (open field test, hanging wire test) and restored striatal histological features. Additionally, Tica opposed the rotenone effect and markedly obliterated the striatal alpha-synuclein content but enhanced the protein expression of tyrosine hydroxylase and dopamine content. On the molecular level, Tica inhibited striatal endoplasmic reticulum stress (ERS) as evidenced by the downregulation of the ER-resident transmembrane sensor inositol-requiring enzyme 1 alpha and its downstream molecular targets, TNF receptor-associated factor 2 and c-Jun N-terminal kinase, along with a reduction in caspase-3 activity. On the other hand, Tica augmented the autophagy machinery by upregulating the autophagosome markers Beclin-1 and light chain 3-II, while inhibiting the content of cathepsin-D.
	Therefore, the current study is the first to accentuate the neuroprotective potential of Tica in a rat model of PD via modulating the crosstalk between ERS, apoptosis, and autophagy to represent a potential novel therapeutic candidate for managing PD, particularly in patients with or prone to cardiovascular diseases.; ÙØ¹Ø¯ ÙØ±Ø¶ Ø§ÙØ´ÙÙ Ø§ÙØ±Ø¹Ø§Ø´ Ø«Ø§ÙÙ Ø£ÙØ«Ø± Ø§ÙØ§Ø¶Ø·Ø±Ø§Ø¨Ø§Øª Ø§ÙØ¹ØµØ¨ÙØ© Ø§ÙØªÙÙØ³ÙØ© ÙØ§ÙØ°Ù ÙØªÙÙØ² Ø¨Ø§ÙØªÙÙØ³ Ø§ÙÙØ³ØªÙØ± ÙÙØ®ÙØ§ÙØ§ Ø§ÙØ¹ØµØ¨ÙØ© Ø§ÙØ¯ÙØ¨Ø§ÙÙÙÙØ© ÙÙ Ø§ÙÙØ§Ø¯Ø© Ø§ÙØ³ÙØ¯Ø§Ø¡ ÙÙØ§ ÙÙØªØ¬ Ø¹ÙÙÙÙØµÙÙØ¯ÙØ¨Ø§ÙÙÙ Ù ÙØ¤Ø¯Ù Ø¥ÙÙ ØµØ¹ÙØ¨Ø§Øª Ø­Ø±ÙÙØ©. ÙØ°ÙÙ ÙØ¹Ø¯ ÙÙÙØ°Ø¬ Ø§ÙØ±ÙØªÙÙÙÙ ÙÙÙØ°Ø¬Ø§ Ø¬ÙØ¯ÙØ§ ÙÙØ¯Ø±Ø§Ø³Ø§Øª Ø§ÙØªØ¬Ø±ÙØ¨ÙØ©Ø­ÙØ« Ø£Ù Ø§ÙØ³ÙØ§Øª Ø§ÙÙØ±Ø¶ÙØ© ÙÙØ±Ø¶ Ø§ÙØ´ÙÙ Ø§ÙØ±Ø¹Ø§Ø´ Ø§ÙÙØ§Ø¬Ù Ø¹Ù Ø§ÙØ±ÙØªÙÙÙÙ ØªØªØ´Ø§Ø¨Ù Ø¥ÙÙ Ø­Ø¯ ÙØ¨ÙØ± ÙÙ Ø§ÙØ¹Ø¯ÙØ¯ ÙÙ Ø§ÙØ¢ÙÙØ§Øª Ø§ÙØ®Ø§ØµØ© Ø¨ÙØ±Ø¶ Ø§ÙØ´ÙÙ Ø§ÙØ±Ø¹Ø§Ø´ ÙØ§ÙØªÙ ØªØ´ÙÙ Ø¥Ø¹Ø§ÙØ© Ø¥Ø´Ø§Ø±Ø§Øª Ø§ÙØ¥ÙØªÙØ§Ù Ø§ÙØ°Ø§ØªÙ ÙÙØ´Ø§Ø·Ø¥Ø¬ÙØ§Ø¯Ø§ÙØ´Ø¨ÙØ© Ø§ÙØ¥ÙØ¯ÙØ¨ÙØ§Ø²ÙÙØ© ÙØ§ÙÙÙØª Ø§ÙØ®ÙÙÙØ Ø¨Ø§ÙØ¥Ø¶Ø§ÙØ© Ø¥ÙÙ Ø§ÙØ®ÙØ§Ø¶ ÙØ³ØªÙÙØ§Øª Ø§ÙØ¯ÙØ¨Ø§ÙÙÙ ÙØ¥ÙØ²ÙÙ Ø§ÙØªÙØ±ÙØ²ÙÙ ÙÙØ¯Ø±ÙÙØ³ÙÙÙØ²Ø ÙØ²ÙØ§Ø¯Ø© ÙØ³ØªÙÙØ§Øª Ø§ÙØ£ÙÙØ§ Ø³ÙÙÙÙÙÙÙÙÙ.
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