Hypothesized mechanism of coronavirus-induced neuronal damage via oxidative stress and mitochondria dysfunction

Hypothesized mechanism of coronavirus-induced neuronal damage via oxidative stress and mitochondria dysfunction

The hypothesized mechanism of coronavirus-induced neuronal damage via oxidative stress and mitochondria dysfunction. SARS-CoV-2 infection occurs when TMPRSS2 primes the spike proteins for proteolysis, allowing the binding to ACE2. The affinity interaction triggers the binding of Ang II to the angiotensin type 1 receptor (AT1R), activating NADPH oxidase. This leads to mitochondrial electron transport chain (ETC) damage via the release of oxidative and nitrosative species, subsequently increasing the formation of mitochondrial reactive oxygen species (mtROS). The signaling pathways mediated by mtROS trigger the production of inflammatory cytokines, which can compromise the blood–brain barrier, thus resulting in neuronal damage. Additionally, mtROS cause nuclear and mitochondrial damage, which prolongs mitochondrial dysfunction and encourages inflammatory senescence (created with BioRender)

Publication

Ginkgo Biloba and Long COVID: In Vivo and In Vitro Models for the Evaluation of Nanotherapeutic Efficacy (2023) Thelma Akanchise, et al. Pharmaceutics. 2023 May;15(5). Figure: F3.

Gene mentions

Organism	Group	Word	Match	Source	NCBI Symbol	NCBI ID
Homo sapiens	Primates	ACE2	ACE2	ncbigene_symbol	ACE2	59272
Homo sapiens	Primates	TMPRSS2	TMPRSS2	ncbigene_symbol	TMPRSS2	7113
Homo sapiens	Primates	AngII↑	ANG2	ncbigene_synonym	ANGPT2	285
Homo sapiens	Primates	AngII↑	ANG2	ncbigene_synonym	VPS51	738
Homo sapiens	Primates	ECT	ECT	ncbigene_symbol	ECT	100379198
Homo sapiens	Primates	NADPH	NADPH	ncbigene_synonym	DECR1	1666
Homo sapiens	Primates	ATP	ATP	ncbigene_synonym	ATP8A2	51761
Homo sapiens	Primates	PKC	PKC	ncbigene_synonym	PRRT2	112476
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKCA	5578
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKCB	5579
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKCD	5580
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKCE	5581
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKCG	5582
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKCH	5583
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKCI	5584
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKCQ	5588
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKCZ	5590
Homo sapiens	Primates	PKC	PKC	famplex_relations	PRKD3	23683
Homo sapiens	Primates	RAC-1	RAC-1	ncbigene_synonym	RAC1	5879
Homo sapiens	Primates	C-SR	CSR	ncbigene_synonym	MORF4	10934
Homo sapiens	Primates	C-SR	CSR	ncbigene_synonym	SCARA3	51435
Homo sapiens	Primates	TNF-a	TNF-A	ncbigene_synonym	TNF	7124
Homo sapiens	Primates	IL-6	IL-6	ncbigene_synonym	IL6	3569
Homo sapiens	Primates	IL-8	IL8	ncbigene_synonym	CXCL8	3576
Homo sapiens	Primates	IL-1B	IL1B	ncbigene_symbol	IL1B	3553
Homo sapiens	Primates	ADP	ADP	ncbigene_synonym	WDTC1	23038
Homo sapiens	Primates	ALS,	ALS	ncbigene_synonym	IGFALS	3483
Homo sapiens	Primates	ALS,	ALS	ncbigene_synonym	SOD1	6647

Chemical mentions

Word	Match	Name	ChEBI
protein	Protein	a protein	chebi:16541
Angiotensin II	angiotensin II	angiotensin II	chebi:58506
NADPH	NADPH	2'-O-phosphonatoadenosine 5'-{3-[1-(3-carbamoyl-1,4-dihydropyridin-1-yl)-1,4-anhydro-D-ribitol-5-yl] diphosphate}	chebi:57783
ATP	ATP	ATP	chebi:30616
ROS	ROS		chebi:26523
TCA	TCA	trichloroacetic acid	chebi:30956
ADP	ADP	L-alanyl-L-alpha-aspartyl-L-proline	chebi:73342
ATP	ATP	ATP	chebi:30616
ATP	ATP	ATP	chebi:30616

Disease mentions

Word	Match	MeSH	Name	DOID
Dementia	dementia		dementia	DOID:1307