| dc.rights.license | CC-BY-NC-ND | |
| dc.contributor | Ik heb de scriptie in mijn eentje geschreven. Marcel Fens en Massimiliano Caiazzo hebben deze beoordeeld en mij van feedback voorzien. | |
| dc.contributor.advisor | Caiazzo, Massimiliano | |
| dc.contributor.author | Vliet, Emile van | |
| dc.date.accessioned | 2024-06-01T23:01:45Z | |
| dc.date.available | 2024-06-01T23:01:45Z | |
| dc.date.issued | 2024 | |
| dc.identifier.uri | https://studenttheses.uu.nl/handle/20.500.12932/46474 | |
| dc.description.abstract | Parkinson’s disease (PD) is a neurodegenerative disorder where formation of Lewy Bodies (LBs) in the
dopaminergic neurons of the substantial nigra pars compacta (SN) cause progressive cell death,
resulting in a dopamine (DA) deficiency which manifests itself in motor symptoms including tremors
and bradykinesia. Current PD treatments focus on symptom reduction through oral delivery of
levodopa (L-DOPA), a precursor of DA. However, L-DOPA delivery to the brain is inefficient due to low
oral bioavailability, degradation in the gastrointestinal (GI) tract and the liver, short systemic half-life,
systemic L-DOPA decarboxylation into DA and limited brain uptake due to the blood brain barrier
(BBB). Additionally, due to the buildup of L-DOPA tolerance by the PD brain, increased dosages are
required as the disease progresses, resulting in increased systemic DA concentrations causing serious
side effects like dyskinesias. To improve PD treatment efficiency and to reduce side effects, recent
research focuses on the encapsulation of L-DOPA in nanoparticles (NPs), the most popular of which
include the polymeric- and lipid-based NPs. Both formulations are able to protect L-DOPA from
systemic decarboxylation into DA and increase L-DOPA delivery to the central nervous system (CNS).
Additionally, these NPs can be modified with proteins and antibodies specifically targeting the BBB,
not only improving targeting to-, but also the crossing of the BBB, thereby reducing required dosages
and free systemic DA. An alternative treatment strategy is to avoid the BBB altogether through direct
intranasal delivery of NP encapsulated L-DOPA to the brain. Through intranasal delivery, L-DOPA can
be directly delivered to the brain via the olfactory and trigeminal nerves, reducing free systemic DA
and avoiding the BBB-associated problems. These polymeric- and lipid-based NPs can be additionally
modified to improve mucoadhesion and cell penetration, resulting in increased therapeutic
concentrations of DA in all parts of the brain. In this review I will give an overview of the recent
advancements made in the field of PD treatment, regarding NP encapsulated L-DOPA delivery to the
brain via either the oral and IV route, as well as the direct intranasal delivery. | |
| dc.description.sponsorship | Utrecht University | |
| dc.language.iso | EN | |
| dc.subject | De behandeling van Parkinsons met Levodopa, en hoe deze behandeling kan worden verbeterd in de toekomst door Levodopa in polymeren en lipiden nanoparticles te laden, en deze vervolgens intraveneus of intranasaal toe te dienen. Ik heb in deze scriptie de voordelen en nadelen van elk soort nanoparticle uitgebreid behandeld, evenals de delivery routes, en vervolgens mijn eigen mening gegeven over het onderzoek wat nog nodig is om deze behandeling te verbeteren. | |
| dc.title | Levodopa-loaded polymeric- and lipid-based nanoparticles for the treatment of Parkinson’s Disease | |
| dc.type.content | Master Thesis | |
| dc.rights.accessrights | Open Access | |
| dc.subject.keywords | Parkinson's disease, Lipid nanoparticles, polymeric nanoparticles, drug delivery, brain targeting, blood-brain barrier, intranasal brain delivery. | |
| dc.subject.courseuu | Regenerative Medicine and Technology | |
| dc.thesis.id | 14621 | |
