Effects of Intermittent Fasting on Health, Aging, and Disease
New England Journal of Medicine,
Journal Year:
2019,
Volume and Issue:
381(26), P. 2541 - 2551
Published: Dec. 25, 2019
Evidence
is
accumulating
that
eating
in
a
6-hour
period
and
fasting
for
18
hours
can
trigger
metabolic
switch
from
glucose-based
to
ketone-based
energy,
with
increased
stress
resistance,
longevity,
decreased
incidence
of
diseases,
including
cancer
obesity.
Language: Английский
Hallmarks of Brain Aging: Adaptive and Pathological Modification by Metabolic States
Cell Metabolism,
Journal Year:
2018,
Volume and Issue:
27(6), P. 1176 - 1199
Published: June 1, 2018
Language: Английский
Brain energy rescue: an emerging therapeutic concept for neurodegenerative disorders of ageing
Nature Reviews Drug Discovery,
Journal Year:
2020,
Volume and Issue:
19(9), P. 609 - 633
Published: July 24, 2020
Language: Английский
Neurotrophic Factor BDNF, Physiological Functions and Therapeutic Potential in Depression, Neurodegeneration and Brain Cancer
International Journal of Molecular Sciences,
Journal Year:
2020,
Volume and Issue:
21(20), P. 7777 - 7777
Published: Oct. 21, 2020
Brain-derived
neurotrophic
factor
(BDNF)
is
one
of
the
most
distributed
and
extensively
studied
neurotrophins
in
mammalian
brain.
BDNF
signals
through
tropomycin
receptor
kinase
B
(TrkB)
low
affinity
p75
neurotrophin
(p75NTR).
plays
an
important
role
proper
growth,
development,
plasticity
glutamatergic
GABAergic
synapses
modulation
neuronal
differentiation,
it
influences
serotonergic
dopaminergic
neurotransmission.
acts
as
paracrine
autocrine
factor,
on
both
pre-synaptic
post-synaptic
target
sites.
It
crucial
transformation
synaptic
activity
into
long-term
memories.
considered
instructive
mediator
functional
structural
central
nervous
system
(CNS),
influencing
dendritic
spines
and,
at
least
hippocampus,
adult
neurogenesis.
Changes
rate
neurogenesis
spine
density
can
influence
several
forms
learning
memory
contribute
to
depression-like
behaviors.
The
possible
roles
highlighted
this
review
focus
effect
antidepressant
therapies
BDNF-mediated
plasticity.
Moreover,
we
will
data
that
illustrate
a
potent
protective
able
confer
protection
against
neurodegeneration,
particular
Alzheimer’s
disease.
Finally,
give
evidence
how
involvement
pathogenesis
brain
glioblastoma
has
emerged,
thus
opening
new
avenues
for
treatment
deadly
cancer.
Language: Английский
NAD+ in Brain Aging and Neurodegenerative Disorders
Cell Metabolism,
Journal Year:
2019,
Volume and Issue:
30(4), P. 630 - 655
Published: Oct. 1, 2019
NAD+
is
a
pivotal
metabolite
involved
in
cellular
bioenergetics,
genomic
stability,
mitochondrial
homeostasis,
adaptive
stress
responses,
and
cell
survival.
Multiple
NAD+-dependent
enzymes
are
synaptic
plasticity
neuronal
resistance.
Here,
we
review
emerging
findings
that
reveal
key
roles
for
related
metabolites
the
adaptation
of
neurons
to
wide
range
physiological
stressors
counteracting
processes
neurodegenerative
diseases,
such
as
those
occurring
Alzheimer's,
Parkinson's,
Huntington
amyotrophic
lateral
sclerosis.
Advances
understanding
molecular
mechanisms
NAD+-based
resilience
will
lead
novel
approaches
facilitating
healthy
brain
aging
treatment
neurological
disorders.
Nicotinamide
adenine
dinucleotide
(NAD+)
fundamental
molecule
health
disease,
it
central
several
bioenergetic
functions.
synthesized
via
three
major
pathways,
including
de
novo
biosynthesis,
Preiss-Handler
pathway,
salvage
pathway
(Figure
1).
While
aspartate
most
photosynthetic
eukaryotes,
kynurenine
only
synthetic
mammals.
The
starts
with
catabolism
amino
acid
tryptophan
converted
two
steps
intermediate
kynurenine,
which
can
generate
NAD+,
kynurenic
acid,
or
xanthurenic
(Vécsei
et
al.,
2013Vécsei
L.
Szalárdy
Fülöp
F.
Toldi
J.
Kynurenines
CNS:
recent
advances
new
questions.Nat.
Rev.
Drug
Discov.
2013;
12:
64-82Crossref
PubMed
Scopus
(263)
Google
Scholar).
modulates
functions
synthesis
neurotransmitters
(glutamate
acetylcholine)
well
regulates
N-methyl-D-aspartate
(NMDA)
receptor
activity
free
radical
production
exhibits
"double-edged
sword"
effects
on
both
neuroprotective
(tryptophan,
picolinic
acid)
neurotoxic
intermediates,
3-hydroxykynurenine
(3-HK)
generates
radicals,
3-hydroxyanthranilic
(3-HAA),
quinolinic
(that
induces
glutamate
excitotoxicity)
an
NMDA
antagonist,
agonist
ambient
levels
these
determined
by
different
enzymes,
preferentially
localized
microglia
astrocytes,
suggesting
necessary
glial
cell-neuron
communication
(Schwarcz
Pellicciari,
2002Schwarcz
R.
Pellicciari
Manipulation
kynurenines:
targets,
effects,
clinical
opportunities.J.
Pharmacol.
Exp.
Ther.
2002;
303:
1-10Crossref
(399)
synthesize
from
pyridine
bases.
synthesizes
nicotinic
(NA)
(NAAD).
One
important
step
constitutes
nicotinamide
mononucleotide
adenylyltransferases
(NMNATs),
also
pathways.
Three
mammalian
NMNATs
exist,
NMNAT1–3,
showing
mice
D.
melanogaster
models
(Ali
2013Ali
Y.O.
Li-Kroeger
Bellen
H.J.
Zhai
R.G.
Lu
H.C.
NMNATs,
evolutionarily
conserved
maintenance
factors.Trends
Neurosci.
36:
632-640Abstract
Full
Text
PDF
(0)
NMNAT1
NMNAT3
ubiquitously
expressed,
NMNAT2
enriched
brain,
adequate
seem
be
essential
axon
development
survival
(Gilley
2019Gilley
Mayer
P.R.
Yu
G.
Coleman
M.P.
Low
compromise
survival.Hum.
Mol.
Genet.
2019;
28:
448-458Crossref
(4)
recycling
(NAM)
(NMN)
intracellular
phosphoribosyltransferase
(iNAMPT),
followed
conversion
NMN
into
(Bogan
Brenner,
2008Bogan
K.L.
Brenner
C.
Nicotinic
nicotinamide,
riboside:
evaluation
precursor
vitamins
human
nutrition.Annu.
Nutr.
2008;
115-130Crossref
(269)
Scholar,
Verdin,
2015Verdin
E.
NAD(+)
aging,
metabolism,
neurodegeneration.Science.
2015;
350:
1208-1213Crossref
(234)
Additionally,
riboside
(NR)
integrates
this
NR
kinase
1
(NRK1)
NRK2
(Bieganowski
2004Bieganowski
P.
Discoveries
nutrient
NRK
genes
establish
independent
route
fungi
humans.Cell.
2004;
117:
495-502Abstract
(315)
Ratajczak
2016Ratajczak
Joffraud
M.
Trammell
S.A.
Ras
Canela
N.
Boutant
Kulkarni
S.S.
Rodrigues
Redpath
Migaud
M.E.
al.NRK1
controls
metabolism
cells.Nat.
Commun.
2016;
7:
13103Crossref
(82)
Despite
NAMPT
being
relatively
highly
expressed
brown
adipocyte,
liver,
kidney
tissues
compared
tissue
mice,
studies
have
supported
role
iNAMPT
(Stein
Imai,
2014Stein
L.R.
Imai
S.
Specific
ablation
Nampt
adult
neural
stem
cells
recapitulates
their
functional
defects
during
aging.EMBO
2014;
33:
1321-1340PubMed
Stein
Wozniak
D.F.
Dearborn
J.T.
Kubota
Apte
R.S.
Izumi
Y.
Zorumski
C.F.
Expression
hippocampal
cortical
excitatory
critical
cognitive
function.J.
34:
5800-5815Crossref
Zhang
2010Zhang
W.
Xie
Wang
T.
Bi
Li
H.
L.Q.
Ye
S.Q.
Ding
Neuronal
protective
PBEF
mouse
model
cerebral
ischemia.J.
Cereb.
Blood
Flow
Metab.
2010;
30:
1962-1971Crossref
(62)
Experimental
evidence
suggests
blood
NA
NAM
able
cross
plasma
membrane,
while
cannot
taken
up
directly
but
needs
smaller
uncharged
molecules
enter
(Hara
2007Hara
Yamada
K.
Shibata
Osago
Hashimoto
Tsuchiya
Elevation
NAD
involvement
cells.J.
Biol.
Chem.
2007;
282:
24574-24582Crossref
(104)
Extracellularly,
digested
membrane-bound
CD38
CD157,
further
metabolized
extracellular
(eNAMPT);
however,
CD73
ways
been
proposed.
First,
converts
CD73,
presumptive
nucleoside
transporter
(Fletcher
2017Fletcher
Doig
C.L.
Oakey
L.A.
Callingham
Da
Silva
Xavier
Garten
A.
Elhassan
Y.S.
al.Nicotinamide
kinases
display
redundancy
mediating
skeletal
muscle
cells.Mol.
2017;
6:
819-832Crossref
(11)
Grozio
2013Grozio
Sociali
Sturla
Caffa
I.
Soncini
Salis
Raffaelli
De
Flora
Nencioni
Bruzzone
protein
source
precursors
sustained
biosynthesis
FK866-treated
tumor
288:
25938-25949Crossref
(55)
Nikiforov
2011Nikiforov
Dölle
Niere
Ziegler
Pathways
subcellular
compartmentation
cells:
entry
generation.J.
2011;
286:
21767-21778Crossref
(154)
2016Sociali
Raffaghello
Magnone
Zamporlini
Emionite
Bianchi
Vigliarolo
Nahimana
al.Antitumor
effect
combined
inhibition
ovarian
cancer
model.Oncotarget.
2968-2984Crossref
(16)
Second,
may
metabolize
NMN,
not
NR,
NAM,
membrane
(Camacho-Pereira
2016Camacho-Pereira
Tarragó
M.G.
Chini
C.C.S.
Nin
V.
Escande
Warner
G.M.
Puranik
A.S.
Schoon
R.A.
Reid
J.M.
Galina
al.CD38
dictates
age-related
decline
dysfunction
through
SIRT3-dependent
mechanism.Cell
23:
1127-1139Abstract
(112)
Sauve
1998Sauve
A.A.
Munshi
Lee
Schramm
V.L.
reaction
mechanism
CD38.
A
single
responsible
cyclization,
hydrolysis,
base-exchange
chemistries.Biochemistry.
1998;
37:
13239-13249Crossref
(83)
Third,
has
reported
(Grozio
2019Grozio
Mills
K.F.
Yoshino
Tokizane
Lei
Cunningham
Sasaki
al.Slc12a8
transporter.Nat.
1:
47-57Crossref
(88)
2011Yoshino
Yoon
M.J.
mononucleotide,
intermediate,
treats
pathophysiology
diet-
age-induced
diabetes
mice.Cell
14:
528-536Abstract
(442)
newly
transporter,
Slc12a8,
regulated
murine
small
intestine,
Slc12a8
deficiency
abrogates
uptake
vitro
vivo
These
pathways
detailed
Figure
1.
Studies
humans
indicate
supplementation
dramatically
upregulates
NAAD,
unknown
metabolic
possibilities
NAAD
and/or
(NAMN)
(Trammell
2016aTrammell
Schmidt
M.S.
Weidemann
B.J.
Jaksch
Dellinger
R.W.
Z.
Abel
E.D.
uniquely
orally
bioavailable
humans.Nat.
12948Crossref
(131)
Thus,
although
intensively
characterized
long
time,
there
remaining
determined.
vital
redox
cofactor
ATP
production,
substrate
at
least
four
families
healthspan
longevity
(Fang
2017Fang
E.F.
Lautrup
Hou
Y.J.
Demarest
T.G.
Croteau
D.L.
Mattson
Bohr
V.A.
aging:
translational
implications.Trends
Med.
899-916Abstract
Gomes
2013Gomes
A.P.
Price
N.L.
Ling
A.J.
Moslehi
J.J.
Montgomery
M.K.
Rajman
White
J.P.
Teodoro
J.S.
Wrann
C.D.
Hubbard
B.P.
al.Declining
pseudohypoxic
state
disrupting
nuclear-mitochondrial
aging.Cell.
155:
1624-1638Abstract
(529)
plays
glycolysis
citric
(TCA)
cycle,
its
ability
accept
hydride
equivalents,
forming
NADH
(Krebs,
1970Krebs
H.A.
Rate
control
tricarboxylic
cycle.Adv.
Enzyme
Regul.
1970;
8:
335-353Crossref
Wallace,
2012Wallace
D.C.
Mitochondria
cancer.Nat.
Cancer.
2012;
685-698Crossref
(853)
one
electron
donors
oxidative
phosphorylation
(OXPHOS)
mitochondria,
providing
electrons
transport
chain
(ETC)
ratio
NAD+/NADH
various
reactions
compartments,
increased
influence
homeostasis
changes
(Ying,
2008Ying
NADP+/NADPH
death:
regulation
biological
consequences.Antioxid.
Redox
Signal.
10:
179-206Crossref
(649)
functions,
antioxidation
generation
stress,
calcium
death
In
addition
NAD+-consuming
proteins,
catabolize
NAM.
They
class
III
histone
deacetylases
sirtuins
(SIRTs),
poly
(ADP-ribose)
polymerases
(PARPs),
ADP
ribosyl-cyclases
(CD38/CD157),
NADase
sterile
alpha
TIR
motif-containing
(SARM1)
mammals,
seven
SIRTs,
regulate
large
number
survival,
rejuvenation,
cancer,
(Chalkiadaki
Guarente,
2015Chalkiadaki
Guarente
multifaceted
15:
608-624Crossref
(150)
SIRTs
spectrum
disease
2000Imai
Armstrong
C.M.
Kaeberlein
Transcriptional
silencing
Sir2
NAD-dependent
deacetylase.Nature.
2000;
403:
795-800Crossref
(2280)
For
example,
SIRT1
consumes
glycolysis,
gluconeogenesis,
balance
between
biogenesis
mitophagy
responses
exercise
metabolic/excitatory
challenges
(Bonkowski
Sinclair,
2016Bonkowski
Sinclair
D.A.
Slowing
ageing
design:
rise
sirtuin-activating
compounds.Nat.
Cell
17:
679-690Crossref
Cheng
2016Cheng
Yang
Zhou
Maharana
Peng
Liu
Wan
Marosi
Misiak
al.Mitochondrial
SIRT3
mediates
challenges.Cell
128-142Abstract
(98)
Fang,
2019Fang
Mitophagy
inhibit
Alzheimer
disease.Autophagy.
1112-1114Crossref
(2)
Furthermore,
shown
promote
neurite
outgrowth
development,
regulating
dendritic
arborization,
long-term
potentiation
learning,
memory
(Gao
2010Gao
W.Y.
Mao
Y.W.
Gräff
Guan
Pan
Mak
Kim
Su
S.C.
Tsai
L.H.
miR-134.Nature.
466:
1105-1109Crossref
(585)
Among
17
PARPs,
them
capable
adding
multiple
ADP-ribose
units
(poly[ADP-ribosyl]ation)
PARylation;
they
PARP1,
PARP2,
PARP5a
(tankyrase
1),
PARP5b
2)
(Leung,
2017Leung
A.K.L.
PARPs.Curr.
27:
R1256-R1258Abstract
Rouleau
2010Rouleau
Patel
Hendzel
Kaufmann
S.H.
Poirier
G.G.
PARP
inhibition:
PARP1
beyond.Nat.
293-301Crossref
(813)
supports
transfers
first
moiety
lysine,
arginine,
glutamate,
aspartate,
serine
residues
acceptor
protein,
preceding
ones,
thereby
poly(ADP-ribose)
(PAR)
chains
(Bonfiglio
2017Bonfiglio
Fontana
Q.
Colby
Gibbs-Seymour
Atanassov
Bartlett
Zaja
Ahel
Matic
Serine
ADP-ribosylation
depends
HPF1.Mol.
Cell.
940:
932-940Abstract
Daniels
2014Daniels
Ong
S.E.
Leung
A.K.
Phosphoproteomic
approach
characterize
mono-
poly(ADP-ribosyl)ation
sites
Proteome
Res.
13:
3510-3522Crossref
(74)
majority
PARylation
executed
participates
processes,
DNA
repair,
DNA/RNA
response.
PAR
serving
signaling
scaffolding
element
2016bFang
Scheibye-Knudsen
Chua
Nuclear
damage
signalling
mitochondria
ageing.Nat.
308-321Crossref
Leung,
Scholar),
e.g.,
stabilization
repair
forks,
catalytic
single-strand
breaks,
bulky
lesions,
double-strand
breaks
(DSBs)
(Ray
Chaudhuri
Nussenzweig,
2017Ray
Nussenzweig
chromatin
remodelling.Nat.
18:
610-621Crossref
(33)
However,
excessive
activation
trigger
death,
termed
parthanatos,
formation
triggers
release
apoptosis-inducing
factor
(AIF)
cytosolic
side
outer
membrane.
AIF
then
translocated
nucleus
activate
macrophage
migration
inhibitory
(MIF,
nuclease),
finally
results
MIF-dependent
chromatinolysis
(Wang
2011Wang
N.S.
Haince
J.F.
Kang
David
K.K.
Andrabi
Dawson
T.M.
Poly(ADP-ribose)
binding
polymerase-1-dependent
(parthanatos).Sci.
4:
ra20Crossref
(198)
2016Wang
An
Umanah
G.K.
Park
Nambiar
Eacker
S.M.
B.
Bao
Harraz
M.M.
Chang
al.A
nuclease
induced
polymerase-1.Science.
354Crossref
(65)
2002Yu
S.W.
Poitras
M.F.
Coombs
Bowers
W.J.
Federoff
Mediation
factor.Science.
297:
259-263Crossref
(1386)
Notably,
depletion
PAR-dependent
hexokinase
activity,
resulting
dysfunctional
likely
(Andrabi
2014Andrabi
Stevens
Karuppagounder
Gagné
polymerase-dependent
energy
occurs
glycolysis.Proc.
Natl.
Acad.
Sci.
USA.
111:
10209-10214Crossref
(128)
Fouquerel
2014Fouquerel
Goellner
E.M.
Barbi
Moura
Feinstein
Wheeler
Romero
al.ARTD1/PARP1
negatively
inhibiting
depletion.Cell
Rep.
1819-1831Abstract
loss,
hyperactivation
PARP1-induced
induce
loss
accelerated
2016aFang
Kassahun
Shamanna
Kalyanasundaram
Bollineni
R.C.
Wilson
M.A.
al.NAD(+)
replenishment
improves
lifespan
ataxia
telangiectasia
repair.Cell
24:
566-581Abstract
view
detrimental
endogenous
exogenous
excitotoxicity,
ischemia-reperfusion
injury,
inflammation-induced
(Yu
Scholar)
targeting
provide
therapeutic
strategies
diseases.
catalyzes
Ca2+-responsive
messenger
cyclic
(cADPR)
use
immunity,
inflammation,
even
social
behaviors
(Jin
2007Jin
H.X.
Hirai
Torashima
Nagai
Lopatina
O.
Shnayder
N.A.
Noda
Seike
behaviour
oxytocin
secretion.Nature.
446:
41-45Crossref
(395)
type
II
form
(i.e.,
C-terminal)
(with
domain
facing
cytosol)
(Liu
2017Liu
Zhao
W.H.
Y.N.
Z.Y.
Fang
S.L.
Cytosolic
interaction
CIB1
levels.Proc.
2008Liu
Graeff
Kriksunov
I.A.
Lam
Hao
Conformational
closure
site
(dagger)
(double
dagger).Biochemistry.
47:
13966-13973Crossref
age-dependent
increase
CD38,
contribute
impaired
function
lymphocyte
differentiation
antigen,
(Mizuguchi
1995Mizuguchi
Otsuka
Sato
Ishii
Kon
Nishina
Katada
Ikeda
localization
antigen
brain.Brain
1995;
697:
235-240Crossref
(57)
knockout
show
significant
protection
against
ischemic
(Long
2017Long
J.H.
Klimova
Fowler
Loane
D.J.
Kristian
despite
high
level
poly-ADP-ribosylation.Neurochem.
42:
283-293Crossref
(1)
SARM1
recognized
cleaves
ADPR,
cADPR
domain.
It
non-brain
tissues,
liver
(Essuman
2017Essuman
Summers
D.W.
X.
DiAntonio
Milbrandt
toll/interleukin-1
possesses
intrinsic
cleavage
promotes
pathological
axonal
degeneration.Neuron.
93:
1334-1343Abstract
(18)
An,
2018Pan
Z.G.
X.S.
deletion
restrains
NAFLD
fat
diet
(HFD)
reducing
lipid
accumulation.Biochem.
Biophys.
2018;
498:
416-423Crossref
(7)
cyclase
glycohydrolase
activities,
estimated
Michaelis
constant
(Km)
24
μM,
similar
other
known
NAD+-consumers
(PARP1,
50–97
μM;
SIRT1,
94–96
15–25
μM)
(Cantó
2015Cantó
Menzies
K.J.
Auwerx
homeostasis:
balancing
act
nucleus.Cell
22:
31-53Abstract
degeneration
therefore
potential
target
intervention
holds
signal,
clear.
SIRTS,
CD38/CD157,
compete
each
consume
NAD+;
thus,
enzyme
impair
activities
enzymes.
interrelationships
reviewed
recently
equilibrium
synthesis,
consumption,
cytoplasm,
nucleus,
Golgi
apparatus.
Two
expression
subcellular-specific
NAD+-synthetic
transporters
metabolites.
convert
NAD+.
include
Language: Английский
Mitochondrial dysfunction in Alzheimer's disease: Role in pathogenesis and novel therapeutic opportunities
British Journal of Pharmacology,
Journal Year:
2019,
Volume and Issue:
176(18), P. 3489 - 3507
Published: Jan. 24, 2019
Dysfunction
of
cell
bioenergetics
is
a
common
feature
neurodegenerative
diseases,
the
most
which
Alzheimer's
disease
(AD).
Disrupted
energy
utilization
implicates
mitochondria
at
its
nexus.
This
review
summarizes
some
evidence
that
points
to
faulty
mitochondrial
function
in
AD
and
highlights
past
current
therapeutic
development
efforts.
Classical
neuropathological
hallmarks
(β-amyloid
τ)
sporadic
risk
genes
(APOE)
may
trigger
disturbance,
yet
dysfunction
incite
pathology.
Preclinical
clinical
efforts
have
overwhelmingly
centred
on
amyloid
pathway,
but
trials
reveal
clear-cut
benefits.
therapies
aimed
are
few
concentrate
reversing
oxidative
stress
death
pathways.
Novel
research
boosting
bioenergetic
offer
an
alternative
treatment
strategy.
Enhancing
preclinical
models
yield
widespread
favourable
effects
could
benefit
persons
with
AD.
LINKED
ARTICLES:
article
part
themed
section
Therapeutics
for
Dementia
Disease:
New
Directions
Precision
Medicine.
To
view
other
articles
this
visit
http://onlinelibrary.wiley.com/doi/10.1111/bph.v176.18/issuetoc.
Language: Английский
Mitophagy and Neuroprotection
Trends in Molecular Medicine,
Journal Year:
2019,
Volume and Issue:
26(1), P. 8 - 20
Published: July 30, 2019
Language: Английский
Intermittent Fasting in Cardiovascular Disorders—An Overview
Bartosz Malinowski,
No information about this author
Klaudia Zalewska,
No information about this author
Anna Węsierska
No information about this author
et al.
Nutrients,
Journal Year:
2019,
Volume and Issue:
11(3), P. 673 - 673
Published: March 20, 2019
Intermittent
fasting
is
a
form
of
time
restricted
eating
(typically
16
h
and
8
eating),
which
has
gained
popularity
in
recent
years
shows
promise
as
possible
new
paradigm
the
approach
to
weight
loss
reduction
inflammation,
many
potential
long
term
health
benefits.
In
this
review,
authors
will
incorporate
aspects
fasting,
mainly
focusing
on
its
effects
cardiovascular
system,
involving
atherosclerosis
progression,
benefits
for
diabetes
mellitus
type
2,
lowering
blood
pressure,
exploring
other
risk
factors
(such
lipid
profile
inflammation).
Language: Английский
Scientific evidence of diets for weight loss: Different macronutrient composition, intermittent fasting, and popular diets
Nutrition,
Journal Year:
2019,
Volume and Issue:
69, P. 110549 - 110549
Published: July 4, 2019
Language: Английский
The gut metabolite indole-3 propionate promotes nerve regeneration and repair
Elisabeth Serger,
No information about this author
L. Gutiérrez,
No information about this author
Jessica Chadwick
No information about this author
et al.
Nature,
Journal Year:
2022,
Volume and Issue:
607(7919), P. 585 - 592
Published: June 22, 2022
Language: Английский
