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Showing 1 to 7 of 7 (0.408 seconds)Spelling suggestions: "subject:"dissertations -- aphysiological sciences"" "subject:"dissertations -- atphysiological sciences""
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Cell death in hyppxic injury : signaling mechanisms and dynamics in the decision making processLoos, Benjamin 12 1900 (has links)
Thesis (PhD (Physiological Sciences))--University of Stellenbosch, 2009 / ENGLISH ABSTRACT: Three main morphologies of cell death have been described in the diseased
myocardium, type I, better known as apoptotic cell death, which is characterized by
cell shrinkage and chromatin condensation, type II, or cell death with autophagy,
presents a morphology with intracellular accumulation of autophagic vacuoles and
type III, better known as necrosis, is characterized by cellular swelling and rapid
loss in cellular membrane integrity. However, recent literature strongly argues
against rigid classifications in the context of cell death mechanisms but rather
suggests to adopt a view of cell death as a dynamic and integrative cellular
response. Furthermore, the contribution of autophagy in cell death or cell survival
is still poorly understood. Therefore the aims of this study were twofold: (i) to
characterize the contribution of each cell death type in context of the severity and
duration of an ischaemic insult and (ii) to determine whether manipulation of the
autophagic pathway affects the contribution of cell death and translates into
protection of the heart.
Rodent derived cardiac myoblast cells were grown in Dulbecco’s Modified Eagle’s
Medium (DMEM) supplemented with 10% fetal bovine serum (FBS), and incubated
under 5% CO2 conditions. Cells were submitted to protocols of 2, 4 and 8 hrs of
simulated ischaemia (SI) under hypoxic conditions in a humidified environment
containing 0.1% O2, 5% CO2 and the balance N2, followed by 1 hr of reperfusion
respectively. We employed a modified ischaemic buffer containing either 2-deoxy-
D-glucose, sodium dithionate or both, with the aim to create an ischaemic insult of
mild (mild SI), moderate (moderate SI) and severe (severe SI) character
respectively.
We evaluated the contribution of each cell death mode using a combination of
viability- and ATP assays. Molecular markers for each cell death process such as
LC3, PARP and HMGB1 were evaluated using 3-dimensional fluorescence
techniques as well as western blot analysis and flow cytometry. Next, autophagy was induced or inhibited prior to the ischaemic insult, using rapamycin and 3MA
respectively, and similar parameters were evaluated after 2 hours of mild or
moderate SI. Propidium Iodide exclusion and Fluorescence Resonance Energy
Transfer (FRET) in combination with mitochondrial inner membrane depolarization
were employed to assess the onset of cell death dynamically. Flow cytometry was
employed to evaluate the degree of protection. In addition, the ATP levels and
reactive oxygen species (ROS) were evaluated.
Our results strongly indicate a differential induction of cell death, which is
dependent on the severity and duration of the ischaemic insult. Mild SI led to the
induction of autophagy and apoptosis, whilst moderate or severe SI induced both
apoptotic and necrotic cell death without an indication of autophagy. Only mild SI,
but not moderate and severe SI, resulted in an ATP surge.
Moreover, our data provide direct evidence that increased autophagy delays the
loss of cellular membrane integrity and delays caspase-3 activation as well as
mitochondrial depolarization in ischaemic cardiomyocytes. Our results show a
profound effect of increased autophagy on the onset of apoptosis as well as
necrosis under simulated ischaemic conditions, providing cellular protection. This
ATP surge observed during mild SI was abolished with increased autophagy.
Furthermore, our results indicate a profound effect of autophagy on ROS
generation. Under normoxic conditions, increased autophagy induced a significant
decrease in ROS while the inhibition of autophagy significantly increased ROS
generation. However, when increasing or decreasing autophagy prior to the
ischaemic insult, ROS increased significantly in both scenarios.
The results suggest that the severity of ischaemia determines the mode of cell
death differentially. An increase in autophagic responsiveness and flux, as induced
through rapamycin treatment, provides a selective advantage for tissue against
injury, possibly by maintaining intracellular ATP levels through the provision of
metabolic substrates. Autophagy is described as an inherent cellular mechanism
v
which affects the onset of cell death and exhibits protective effects in the ischaemic
myocardium when upregulated prior to the ischaemic insult.
The protective effect of increased autophagy was mirrored in the isolated perfused
rat heart model, reflected by improved functional recovery during
ischaemia/reperfusion. / AFRIKAANSE OPSOMMING: Die drie belangrikste morfologiese beskrywings van seldood in die hart sluit die
volgende in: tipe I, beter bekend as apoptose wat gekenmerk word deur
selkrimping en chromatienkondensering, tipe II, of seldood deur middel van
autofagie wat gekenmerk word deur die intrasellulêre versameling van autofagiese
vakuole en tipe III, beter bekend as nekrose wat gekenmerk word deur sel swelling
en ‘n vinnige verlies aan membraanintegriteit. Onlangse literatuur waarsku egter
teen die onbuigsame klassifikasie van seldoodmeganismes en stel voor dat
seldood as ‘n dinamiese proses met integrerende sellulêre meganismes beskou
moet word. Die bydrae van autofagie in seldoodmeganismes word ook nog nie
goed verstaan nie. Die doel van hierdie studie is dus tweevoudig: (i) om die bydrae
van elke tipe seldood te bepaal in konteks van die felheid en tydperk van die
iskemiese ingryping en (ii) om te bepaal of the manupilering van autofagie ‘n
betekenisvolle bydrae lewer in seldoodmeganismes en sodoende tot beskerming
van die hart kan lei.
Kardiale mioblaste wat van rotweefsel afkomstig is, is in Dulbecco se
gemodifiseerde Eagle medium (DMEM), waarby daar 10% fetale kalfserum gevoeg
is en wat onderhewig was aan 5% CO2 toestande, onderhou. Selle was
onderhewig aan protokolle van 2, 4 en 8 ure gesimuleerde iskemie (SI) onder
hipoksiese toestande in ‘n humiditeitsomgewing wat 0.1% O2, 5% CO2 en die
balans N2 bevat. Daarna was die selle onderhewig aan 1 uur reperfusie. ‘n
Gemodifiseerde iskemiese buffer wat óf 2-deoksie-D-glukose óf natriumdithionaat,
of beide bevat, is gebruik om lig, matig en strawwe iskemiese toestande na te
boots. Die bydrae van elke tipe seldood is geëvalueer tydens bogenoemde toestande
deur gebruik te maak van ‘n kombinasie van sellewensvatbaarheid- en ATP
tegnieke. Molekulêre merkers, wat LC3, PARP en HMGB1 insluit, is gebruik om
deur middel van 3-dimensionele fluoresensie tegnieke, westelike kladtegnieke en
vii
vloeisitometrie die verskillende vorme van seldood te ondersoek. Autofagie is ook
geïnduseer en geïnhibeer voor die iskemiese ingryping, deur middel van
rapamycin en 3MA, respektiewelik om die rol van autofagie tydens seldood te
bepaal. Propidium iodite uitluiting en fluoresensie resonansie energie oordrag
(FRET) in kombinasie met ‘n merker vir mitochondriale binneste membraan
depolarisasie is gebruik om die aanvang van seldood dinamies te ondersoek.
Vloeisitometrie is gebruik om die graad van beskerming aan te dui, terwyl
intrasellulêre ATP vlakke en reaktiewe suurstof spesies (ROS) ook gemeet is.
Ons resultate het getoon dat daar ‘n differensiële indusering van seldood plaasvind
wat afhanklik is van die felheid en tydsduur van die iskemiese ingryping. ‘n Ligte
graad van iskemie lei tot die indusering van autofagie en apoptose, terwyl matige
en strawwe iskemie beide apoptose en nekrose induseer sonder autofagie. Verder
het slegs ‘n ligte graad van iskemie ‘n skerp styging in ATP tweeggebring, terwyl
dit nie die geval was tydens matige en strawwe iskemie nie.
Ons data verskaf ook direkte bewyse dat ‘n toename in autofagie die verlies van
sellulêre membraanintegriteit vertraag. Dit het ook ‘n vermindering in caspase-3
aktivering en mitochondriale depolarisasie in iskemiese kardiomiosiete
teweegebring. Die data dui aan dat ‘n toename in autofagie ‘n beduidende effek op
apoptose en nekrose tydens gesimuleerde iskemiese toestande het om sodoende
selbeskerming te verskaf. Die skerp styging in ATP wat tydens die ligte graad van
iskemie teweeggebring is, is opgehef met ‘n toename in autofagie. Ons resultate
dui ook daarop dat autofagie ‘n beduidende rol in ROS generering speel. Onder
normoksiese omstandighede veroorsaak ‘n toename in autofagie ‘n insiggewende
afname in ROS generering, terwyl die inhibisie van autofagie ROS generering
insiggewend laat toeneem. Wanneer autofagie egter voor die iskemiese ingryping
verhoog of verlaag word, vermeerder ROS generering in beide gevalle.
Hierdie resultate bewys dat die graad van iskemie ‘n invloed het op die tipe
seldood wat geïnduseer word. ‘n Toename in autofagie reaksietyd en vloei, soos
viii
bewerkstellig deur rapamycin, verskaf ‘n selektiewe voordeel vir weefsel teen
beskadiging, heel waarskynlik deur die handhawing van intrasellulêre ATP-vlakke
deur die verskaffing van metaboliese substrate. Autofagie word beskryf as ‘n
inherente sellulêre meganisme wat seldood beïnvloed en die iskemiese
miokardium beskerm wanneer dit opgereguleer word voor die iskemiese ingryping.
Hierdie beskermende rol van autofagie wat in die weefselkultuur waargeneem is, is
ook in die geïsoleerde geperfuseerde rot hart model waargeneem, waar
funksionele herstel verbeter is tydens iskemie/reperfusie.
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Hyperglycemia-induced activation of the hexosamine biosynthetic pathway causes myocardial cell deathRajamani, Uthra 12 1900 (has links)
Thesis (PhD (Physiological Sciences))--University of Stellenbosch, 2009. / ENGLISH ABSTRACT: OBJECTIVE – Oxidative stress increases flux through the hexosamine biosynthetic pathway
(HBP) resulting in greater O-GlcNAcylation of target proteins. Since increased oxidative stress
and HBP flux are associated with insulin resistance, we hypothesized that its activation leads to
greater O-GlcNAcylation of BAD (pro-apoptotic) and increased myocardial apoptosis.
RESEARCH DESIGN AND METHODS – To investigate our hypothesis, we employed two
experimental models: 1) H9c2 cardiomyoblasts exposed to high glucose (33 mM glucose) ± HBP
modulators ± antioxidant treatment vs. matched controls (5.5 mM glucose); and 2) a rat model of
high fat diet-induced insulin resistance and hyperglycemia. We evaluated apoptosis in vitro by
Hoechst nuclear staining, Annexin-V staining, caspase activity measurements and
immunoblotting while in vivo apoptosis was assessed by immunoblotting. In vitro reactive
oxygen species (ROS) levels were quantified by H2DCFDA staining (fluorescence microscopy,
flow cytometry). We determined overall and BAD O-GlcNAcylation, both by immunoblotting
and immunofluorescence microscopy. As BAD-Bcl-2 dimer formation enhances apoptosis, we
performed immunoprecipitation analysis and immunofluorescence microscopy (co-localization)
to determine BAD-cl-2 dimerization. In vivo overall O-GlcNAcylation, BAD O-GlcNAcylation
and BAD-Bcl-2 dimerization was determined by immunoprecipitation and immunoblotting.
4
RESULTS – High glucose treatment of cells significantly increased the degree of apoptosis as
revealed by Hoechst nuclear staining (54 ± 9%, p<0.01 vs. 5.5 mM), Annexin-V staining (43 ±
5%), caspase activity assay (26 ± 2%) and immunoblotting. In parallel, overall OGlcNAcylation
(p<0.001 vs. 5.5 mM), BAD O-GlcNAcylation (p<0.05 vs. 5.5 mM) and ROS
levels were increased (fluorescence microscopy – p<0.05 vs. 5.5 mM; flow cytometry – p<0.001
vs. 5.5 mM). HBP inhibition using DON and antioxidant treatment (α-OHCA) attenuated these
effects while HBP activation by PUGNAc exacerbated it. Likewise, insulin resistant rat hearts
exhibited significantly higher caspase-3 (p<0.05 vs. controls), overall O-GlcNAcylation (p<0.05
vs. controls) and BAD O-GlcNAcylation levels (p<0.05 vs. 5.5 mM). BAD-Bcl-2 dimer
formation was increased in cells exposed to hyperglycemia [immunoprecipitation analysis and
co-localization] and in insulin resistant hearts.
CONCLUSIONS - Our study identified a novel pathway whereby hyperglycemia results in
greater oxidative stress, resulting in increased HBP activation and increased BAD OGlcNAcylation.
We also found greater BAD-Bcl-2 dimerization increasing myocardial
apoptosis, suggesting that this pathway may play a crucial role in the onset of the diabetic
cardiomyopathy. / AFRIKAANSE OPSOMMING: DOELWIT – Oksidatiewe stres verhoog fluks deur die heksosamien biosintetiese weg (HBW)
wat in „n groter O-GlcNAsetilering van teiken proteïene resulteer. Weens die feit dat verhoogde
oksidatiewe stres en HBW fluks verband hou met insulienweerstandigheid, hipotetiseer ons dat
die aktivering hiervan tot groter O-GlcNAsetilering van BAD (pro-aptoptoties) en verhoogde
miokardiale apoptose lei.
NAVORSINGS ONTWERP EN METODES – Om die hipotese te ondersoek het ons twee modelle
ontplooi: 1) H9c2 kardiomioblaste is blootgestel aan hoë glukose konsentrasie (33mM glucose) ±
HBW moduleerders ± antioksidant behandeling vs. gepaarde kontrole (5.5mM glucose); en 2) „n
hoë vet dieetgeïnduseerde insulienweerstandige rotmodel en hiperglukemie. Ons het apoptose in
vitro deur middel van Hoescht nukleuskleuring geëvalueer, kasapase aktiwiteit bepalings en
immunoblotting terwyl apoptose in vivo getoets is deur immunoblotting. Reaktiewe
suurstofspesie (RSS) vlakke is deur middel van H2DCFDA verkleuring (fluoresensie
mikroskopie, vloeisitometrie) bepaal. Algehele en BAD O-GlcNAsetilering is beide deur
immunoblotting en immunofluoresensie mikroskopie bepaal. BAD-Bcl-2 dimeervorming
bevorder apoptose, om BAD-cl-2 dimerisasie te bepaal is daar van immunopresipitering analise
en immunofluoresensie mikroskopie (ko-lokalisasie) gebruik gemaak. In vivo is algehele OGlcNAsetiliering,
BAD O-GlcNAsetiliering en BAD-Bcl-2 dimerisasie deur immunopresipitasie
en immunoblotting bepaal.
6
RESULTE – Hoë glukose behandeling van selle het die graad van apotpose betekenisvol verhoog
soos blootgelê deur Hoechst nukleuskleuring (54 ± 9%, p<0.01 vs. 5.5 mM), Annexin-V kleuring
(43 ± 5%), kaspase aktiviteit assay (26 ± 2%) en immunoblotting. In parallel, algehele OGlcNAsetilering
(p<0.001 vs. 5.5 mM), BAD O-GlcNAsetilering (p<0.05 vs. 5.5 mM) en RSS
vlakke is verhoog (fluoresensie mikroskopie– p<0.05 vs. 5.5 mM; vloeisitometrie– p<0.001 vs.
5.5 mM). HBW inhibering deur van DON en van antioksidant behandeling gebruik te maak (α-
OHCA) het hierdie effekte verlaag terwyl HBW aktivering deur PUGNAc dit verhoog het.
Netso, het insulienweerstandige rotharte betekenisvolle hoë kaspase -3 (p<0.05 vs. kontrole),
algeheel O-GlcNAsetilering (p<0.05 vs. kontrole) en BAD O-GlcNAsetiliering vlakke (p<0.05
vs. 5.5 mM) getoon. BAD-Bcl-2 dimeervorming is verhoog in hiperglukemies blootgestelde selle
[immunopresipitering analise en ko-lokalisering] en in insulienweerstandige harte.
GEVOLGTREKKINGS – Ons studie het „n nuwe weg geïdenifiseer waar hiperglukemie in groter
oksidatiewe stres resulteer wat weer HBW aktivering verhoog en BAD O-GlcNAsetilering
verhoog het. Ons het verder bevind dat groter BAD-Bcl-2 dimerisasie miokardiale apoptose
verhoog wat voorstel dat hierdie weg „n belangrike rol in diabetiese kardiomiopatie speel.
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An integrative approach to the effect of interleukin-6 on adaptation to restraint stress in ratsViljoen, Monet 12 1900 (has links)
Thesis (MSc (Physiological Sciences))--University of Stellenbosch, 2009. / ENGLISH ABSTRACT: Bi-directional communication exists between HPA-axis activation and interleukin-6
(IL-6). However, the relative contribution of centrally versus peripherally secreted IL-
6 remains unclear, especially under psychological stress conditions. We
hypothesised that the HPA response to mild psychological stress is dependent on IL-
6, both centrally and peripherally.
120 male Wistar rats were divided into four groups, depending on whether they
received an anti-IL-6 antibody (Ab) (2μg/ml/kg body weight) or a placebo (sterile
saline) injection and whether or not they were subjected to 1 hour of restraint stress
for 1, 2 or 3 days. Rats were euthanized 24 hours after stress exposure.
Plasma corticosteroid (GC) levels remained significantly increased 24 hours after a
single stress exposure (control placebo (CP) versus stress placebo (SP): p < 0.05).
The undetectable plasma IL-6 levels evident across all groups may be explained by
the short half-life of IL-6. Plasma IL-1β levels decreased when IL-6 was blocked in
unstressed animals (CP versus CAb: p < 0.05), suggesting a role for IL-6 in the
maintenance of IL-1β levels under tonic physiological conditions.
At tissue level, pituitary gland mass increased significantly at time point 2,
independently of stress when blocking IL-6 (CAb: p < 0.05). This suggests that when
normal homeostasis is threatened, immediate adaption or at least compensation
may occur. It was observed that GR, IL-1β, IL-1βR, IL-6, IL-6R and GABAARα1
showed no response to stress alone in the pituitary. It is therefore more likely that
resistance to adaptation exists centrally. IL-1β and IL-1βR (p < 0.05) and
GABAARα1 (p < 0.005) expression increased in the CAb group in the pituitary, again
suggesting a role for IL-6 under control conditions. In terms of the adrenal, blocking IL-6 resulted in decreased glandular mass at time point 1, independent of stress
(CAb and SAb: p < 0.005). The up-regulation in GR expression seen in CAb and
SAb (p < 0.05) may be the effect of a compensatory mechanism to increase IL-6
dependent bioactivity of GCs. The fact that expression of IL-6, IL-6R, IL-1β and IL-
1βR consistently increased in the Ab groups, and mostly in the zona fasciculata and
zona reticularis, suggests that lack of local direct negative cytokine feedback
occurred in response to very low plasma IL-6 levels and that this contributes more
than GCs in the down-regulation of inflammatory cytokine release.
In conclusion, consistent effects of the Ab were apparent in the tissues investigated,
even in control conditions, suggesting that IL-6 plays a role in the maintenance of
basal homeostasis, including its regulation of the response to psychological stress.
We found differential regulation in terms of cytokines and GCs when comparing
peripheral versus central effects of stress and Ab, as well as the levels of cytokines
in the blood compartment, compared to within tissues. / AFRIKAANSE OPSOMMING: Daar bestaan twee-rigting kommunikasie tussen HPA-as aktivering en interleukin-6
(IL-6), allhoewel die relatiewe bydrae van sentraal versus perifeer afgeskeide IL-6
nog onduidelik is, veral gedurende sielkundige strestoestande. Ons hipotese is dat
die HPA reaksie tot sielkundige stres afhanklik van IL-6 is, beide sentraal en in die
periferie.
120 manlike Wistar rotte is in vier groepe verdeel, afhangende van of hulle ‘n anti-IL-
6 teenliggaampie (Ab) (2μg/ml/kg liggaamsgewig) of ‘n plasebo (steriele
soutoplossing) inspuiting gekry het, en of hulle onderworpe was aan 1 uur van
vaskeer-stres vir 1, 2 of 3 dae. Rotte is 24 uur na blootstelling aan stres aan
genadedood onderwerp.
Bloed kortikosteroïed (GC) vlakke het beduidend toegeneem binne 24 uur na ‘n
eenmalige stres blootstelling (kontrole plasebo (CP) versus stres plasebo (SP): p <
0.05). Die onmeetbaar lae vlakke van IL-6 regoor al die groepe, kan verduidelik
word na aanleiding van die kort half-leeftyd van IL-6. Bloed IL-1β vlakke het
afgeneem in kontrole rotte wanneer IL-6 geblok is (CP versus CAb: p < 0.05). Dit kan
beteken dat IL-6 noodsaaklik is vir die onderhoud van IL-1β vlakke gedurende
basale toestande.
Op weefselvlak het die hipofise massa toegeneem by tydpunt 2 toe IL-6 geblok is,
onafhanklik van stres (CAb: p < 0.05). Dit dui aan dat wanneer normale homeostase
bedreig word, daar onmiddelike aanpassing of kompensasie plaasvind. Dit is
opvallend dat GR, IL-1β, IL-1βR, IL-6, IL-6R en GABAARα1 geen respons in terme
van stres alleen in die hipofise getoon het nie. Na aanleiding daarvan is dit meer
waarskynlik dat weerstand tot aanpassing sentraal bestaan. IL-1β and IL-1βR (p <0.05) en GABAARα1 (p < 0.005) uitdrukking in die hipofise het toegeneem in die CAb
groep, wat weereens ‘n rol vir IL-6 onder kontrole toestande uitwys. In terme van die
bynier, het die blok van IL-6 ‘n afname in massa veroorsaak by tydpunt 1, wat weer
onafhanklik van stres was (CAb en SAb: p < 0.005). Die opregulering in die CAb en
SAb groepe (p < 0.05), kan wees as gevolg van ‘n kompensasie meganisme om IL-6
afhanklike GC aktiwiteit te verhoog. Die feit dat die uitdrukking van IL-6, IL-6R, IL-1β
and IL-1βR in die Ab groepe deurlopend verhoog was, en meeste in die zona
fasciculata en zona reticularis, stel voor dat daar ‘n tekort aan plaaslike, direkte
sitokien negatiewe terugvoering was, as gevolg van die merkwaardige lae bloed IL-6
vlakke en dat dit meer bydra as GCs in die afregulering van inflammatoriese sitokien
vrystelling.
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Cytokine super-families affect adult stem cells : IL-6 and the skeletal muscle nicheSteyn, Paul 03 1900 (has links)
Thesis (MSc (Physiological Sciences))--University of Stellenbosch, 2011. / Includes bibliography. / ENGLISH ABSTRACT: Background: IL-6 belongs to a cytokine super-family known to affect cell proliferation,
although other family members are better characterized. Proliferation promoting
factors (IL-6) compete with differentiation promoting factors (myogenic regulatory
factors: MyoD and myogenin) to affect cell cycle. Cell cycle progression is assessed by
determining the proportion of cells shifting from arrest to chromatin synthesis and
mitosis phases (G0/G1 and S and G2/M respectively).
Methods: This study assessed the effects of IL-6 on cell cycle progression and
proliferation vs. differentiation of C2C12 skeletal myoblasts. Physiological doses (10 or
100 pg/ml) were compared to a high dose (10 ng/ml), with exposure lasting 48 hours
(addition of IL-6 dose to proliferation medium at 0 and 24 hours). Acute signaling
downstream of the IL-6 gp130 receptor was assessed after the first exposure.
Results: Propidium iodide analysis of nuclear material using flow cytometry indicated
shifts in forward scatter. Both Low and Medium doses shifted a greater proportion
(p<0.05) of cells from G0/G1 to S and G2M phases at 24 hours and all doses resulted
in the same shift (p<0.05) at the 48 hour time point. However, the High dose
significantly (p<0.05) increased myogenin expression at the 48 hour time point.
Microscopy indicated that confluence was prevented by low seeding density and did
not influence the result. Cells harvested at 5 minutes post stimulation indicated that
all doses significantly increased STAT3 phosphorylation. 10 minutes post stimulation
the High dose group sustained elevated levels of STAT3 phosphorylation.
Conclusions: Low and medium doses of IL-6 increase proliferation in a muscle
satellite cell line by activating cell division and allowing myoblasts to remain in the
active cell cycle. High doses of IL-6 increase differentiation by mediating upregulation
of myogenic regulatory factors and this is thought to be due to prolonged STAT3
activation. Physiological control of myoblast behaviour by cytokines is evident and
such control would be influenced by the severity of the endogenous cytokine
response to various stimuli. / AFRIKAANSE OPSOMMING: Agtergrond: IL-6 behoort aan n sitokien super-familie bekend vir die affektering van
sel verspreiding, alhoewel ander familie lede beter gekenmerk is. Bevordering van
verspreiding faktore (IL-6) kompeteer met bevordering van differensiasie fatore
(myogenic regulatory factors: MyoD en myogenin) om die sel siklus te affekteer. Sel
siklus progressie word geassesseer deur die bepaling van die proporsie selle wat
verskuif van arrestasie na chromatien sintese en mitose fases (G0/G1 en S en G2/M
onderskeidelik).
Metodes: Hierdie studie het die effekte van IL-6 op die progressie van die sel siklus
geassesseer asook die proliferasie vs. differensiasie van C2C12 skelet spier satelliet
selle. Fisiologiese dosisse (10 en 100 pg/ml) was vergelyk tot n hoog dose (10 ng/ml),
met blywende blootstelling van 48 uur (byvoeging van IL-6 dose tot verspreidings
medium op 0 and 24 uur). Akute sein stroomaf van die IL-6 gp130 reseptor was ook
geassesseer na die eerste blootstelling.
Resultate: Propidium iodide analise van kern materiaal deur vloei sitometrie het
voorwaarts verskuiwing aangedui. Beide Laag and Medium doses het n groter
proporsie (p<0.05) selle verskuif van die G0/G1 tot die S en G2M fases na 24 uur en
alle dosisse het gelei in die selfde verskuiwing (p<0.05) by die 48 huur tyd punt.
Alhoewel die Hoog dose myogenin uitdrukking aansienlik (p<0.05) verhoog het na 48
uur. Mikroskopie het aangedui dat samevloeiing voorkom was deur n lae loting
digtheid en dit het nie resultate geaffekteer nie. Selle wat geoes was 5 minute na
stimulasie het aangedui dat alle dosisse STAT3 fosforilasie laat toeneem het. 10
minute na stimulasie het die Hoog dose groep volgehoue vlakke van STAT3 fosforilasie
besit.
Gevolgtrekkings: Laag en Medium dosisse van IL-6 verhoog verspreiding in n spier
satelliet sel lyn deur die aktivering van sel deling en deur selle toe te laat om in die
aktiewe sel siklus te bly. Hoog dosisse van IL-6 verhoog differensiase deur
bemiddelende opstoot van myogenic regulatory factors en die gedagte is dat dit
bewerkstellig word deur aanhoudende aktivering van STAT3. Fisiologies beheer van
satelliet selle deur sitokiene is duidelik en die beheer sal beinvloed word deur die erns
van die endogene sitokien reaksie op verskillende stimuli.
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Hypothalamic-pituitary-adrenal-axis vs. the sympatho-adrenal medullary system in the acute response to psychological stressJanse van Vuuren, Marthinus 03 1900 (has links)
Thesis (MSc (Physiological Sciences))--University of Stellenbosch, 2011. / Includes bibliography. / ENGLISH ABSTRACT: The hypothalamic-pituitary-adrenal-(HPA) axis has long been closely associated with
psychological stress-induced activation of the adrenal cortex and subsequent glucocorticoid
production. Another, less known peripheral limb of the psychological stress response, is the
sympatho adrenal medullary pathway.
We hypothesized that the sympatho-adrenal medullary system constitutes the primary response
to acute psychological stress, with the HPA-axis functioning as a secondary response. We tested
our hypothesis by manipulating a model of acute mild psychological stress (restraint) by
blocking IL-6, a valuable constituent of the sympatho-adrenal medullary system.
Serum corticosterone concentration increased in response to stress (7 ± 3 vs. 57 ± 4 ng/ml;
P<0.0001), a response attenuated when IL-6 was blocked (17 ± 7 ng/ml). Stress increased
pituitary mass only when IL-6 was blocked (38 ± 3 vs. 65 ± 6 mg; P <0.001). Stress increased
left adrenal mass only in the presence of IL-6 (34 ± 1 vs. 73 ± 8 mg; P <0.00001). Stress did not
influence the circulating levels of TNF-α, IL-1β or IL-6 significantly. IL-1β and TNF-α
concentrations in the unstressed rats were lower when IL-6 was blocked.
We then manipulated the stress model by administering S. frutescens extract to elucidate both the
central and peripheral effects of acute S. frutescens administration on the psychological stress
response.
Restraint caused decreases in hippocampal GR levels when compared to respective controls. S.
frutescens administration and exposure to restraint synergistically decreased hippocampal
GABAAR levels. In addition, exposure to both stress and S. frutescens led to a noteworthy
increase in pituitary mass (P = 0.078), as well as pituitary ACTH levels (P < 0.01). Similarly,
differences in circulating ACTH levels showed an effect of stress on ACTH secretion only in the
presence S. frutescens (P < 0.05). Adrenal mass was significantly increased in S. frutescenstreated
animals that were also exposed to restraint (P < 0.05). Adrenal levels of ACTH showed a
reciprocal trend to pituitary and circulating ACTH levels. No statistically significant differences
were seen in adrenal IL-6 content. However, marked increases in IL-6 levels were seen at this
level with administration of S. frutescens stress exposure and a cumulative increase seen with
both S. frutescens-treatment and stress exposure.
Hippocampal GABAAR, pituitary mass, pituitary ACTH and circulating ACTH levels showed a
similar trend towards a synergistic effect of S. frutescens and restraint in activation of the
psychological stress response, while adrenal ACTH levels showed an inverse trend.
Hippocampal GR did not show any effect of stress or S. frutescens-treatment.
The results from these two experiments indicate that the sympatho-adrenal medullary system
constitutes the primary response to acute mild psychological stress and that the HPA-axis is only
activated during an exacerbated stress response or when the sympatho-adrenal medullary
contribution is inadequate. Furthermore, the acute administration of S. frutescens possibly led to
a functional shift in GABAergic function, resulting in activation of the stress response. The
anecdotal reports of a “docile” effect of S. frutescens most likely results from activation of the
mesolimbic dopaminergic system by the hippocampus and amygdala. These results have
dramatic consequence in GABA-based anxiety-treatments. / AFRIKAANSE OPSOMMING: Die hipotalamo-pituïtêre-adrenale (HPA)-as is lank bekend as ‘n primêre rolspeler in die respons
op emosionele stres en daaropvolgende glukokortikoïed produksie. ‘n Ander, minder bekende
arm van die sielkundige stres respons is die simpatiese bynier-medulla-sisteem.
Ons hipotese was dat die laasgenoemde simpatiese bynier-medulla-sisteem die primêre respons
tot sielkundige stres behartig terwyl die HPA-as ‘n sekondêre respons bied. Ons het ons hipotese
getoets deur die manupilering van ‘n beproefde stres model waar ons IL-6, ‘n waardevolle
rolspeler in die simpatiese bynier-medulla-sisteem, onderdruk het.
In respons op stress, het serum kortikosteroon konsentrasies toegeneem slegs in die
teenwoordigheid van IL-6 (7 ± 3 vs. 57 ± 4 ng/ml; P<0.0001), maar nie wanneer IL-6 onderdruk
is nie (17 ± 7 ng/ml). Stres het ‘n verhoging in hipofise massa teweeggebring slegs tydens die
onderdrukking van IL-6 (38 ± 3 vs. 65 ± 6 mg; P <0.001). Stres het ook linker-byniermassa
verhoog slegs wanneer voldoende IL-6 beskikbaar was (34 ± 1 vs. 73 ± 8 mg; P <0.00001).
Stres alleen het geen invloed gehad op serum IL-1β, IL-6 of TNF-α nie, maar die onderdrukking
van IL-6 het wel ‘n inhiberende effek op basale IL-1β en TNF-α gehad.
Daarna het ons weer eens die stresmodel manipuleer deur die rotte ‘n S. frutescens ekstrak te gee
in ‘n poging om beide die sentrale en perifere effekte daarvan op die sielkundige stres respons te
evalueer.
Stres alleen het gelei tot ‘n afname in GR terwyl ‘n kombinasie van stres en S. frutescens
administrasie tot ‘n afname in GABAARα1 in die hippokampus gelei het. Hierdie kombinasie
het ook tot ‘n merkwaardige toename in hipofise massa (P = 0.078) sowel as ACTH-inhoud van
die hipofise (P < 0.01) gelei. ‘n Soortgelyke patroon is waargeneem betreffende sirkulerende
ACTH en byniermassa met P < 0.05 vir elk. Bynier ACTH inhoud, aan die ander kant, het ‘n
omgekeerd eweredige verhouding met ACTH in die hipofise en in sirkulasie getoon. Bynier IL-
6 inhoud het geen statisties beduidende verskille getoon nie, maar ‘n merkwaardige verhoging is
weereens gesien met ‘n kombinasie van stres en S. frutescens administrasie.
Die soortgelyke tendens wat waargeneem word in GABAAR in die hippokampus, asook
hipofise- en sirkulerende ACTH vlakke, en dui op ‘n samewerkende rol van stres en S. frutescens
in die aktivering van die sielkundige stres respons. GR in die hippokampus toon geen
veranderinge nie. Die resultate van die twee eksperimente dui op ‘n primêre rol van die
simpatiese bynier-medulla-sisteem in die respons op ‘n akute stressor en dat die HPA-as net
geaktiveer word tydens ‘n ooreiste stres reaksie of indien die simpatiese bynier-medulla-sisteem
onderdruk word. Die waargenome “verdowings”-effek van S. frutescens word moontlik deur
aktivering van die mesolimbiese dopamien pad deur die hippokampus en amigdala bewerkstellig.
Die resultate mag ook lei tot die heroorweging van GABA-gebaseerde angs medikasies.
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The association between genotype and BMI, health and lifestyle indicators as well as weight loss outcomes in overweight/obese Caucasian adultsHarbron, Janetta 03 1900 (has links)
Thesis (PhD (Physiological Sciences))--University of Stellenbosch, 2011. / Includes bibliography. / ENGLISH ABSTRACT: Genetic screening to improve obesity treatment outcomes is available despite the lack of conclusive
evidence, specifically for Caucasian South Africans, in this regard.
The aim of this study was to investigate the association between genotype (seven polymorphisms) and
body mass index (BMI), health and lifestyle indicators in a cross-sectional sample of overweight/obese
Caucasian adults (n=133), as well as the association between genotype and weight loss outcomes following
an intervention (n=88) using a quasi experimental study design (time-series). The intervention consisted of
a 24-week conservative weight loss programme that included dietary, physical activity and behavioural
components.
The primary null hypothesis for the cross-sectional sample, namely that there is no association between
genotype and BMI, has not been rejected. A number of the secondary/exploratory hypotheses were
rejected of which the most plausible associations (based on support by the literature and a physiological
basis for the findng) are: 1) the mutant TT homozygotes of the GNB3 C825T polymorphism may have a
higher risk to develop the metabolic syndrome (MetS) as they had significantly higher fasting triglyceride
and glucose levels, a higher number of traits that met the diagnostic cut-off criteria for MetS and higher
number of these subjects was diagnosed with MetS compared to the wild-type C-allele carriers; and 2)
subjects with mutant alleles of either the FTO rs1421085 or rs17817449 polymorphisms may have poorer
eating behaviours (a higher rigid control, habitual and emotional disinhibition, perceived hunger and
internal locus for hunger) and higher intake of high-fat foods.
The primary null hypothesis for the intervention sample, namely that there is no association between
genotype and weight loss outcome, was not rejected for the FABP2 Ala54Thr, INSIG2 rs7566605, FTO
rs1421085, ADRB3 Trp64Arg and GNB3 C825T polymorphisms. However, it was rejected in some instances
indicating the following associations: 1) The wild-type TT homozygotes of the FTO rs17817449
polymorphism lost significantly more weight during the first two months of the program compared to the
mutant allele carriers (this is a novel finding); 2) The wild-type Arg16Arg homozygotes of the ADRB2
Arg16Gly polymorphism lost significantly more weight during the first month of the program compared to
the mutant allele carriers (this finding is supported by one other intervention study); 3) Subjects with a
mutant C-allele of the INSIG2 rs7566605 polymorphism and a mutant Gly16-allele of the ADRB2 Arg16Gly
polymorphism lost significantly less weight over the six month intervention period (this is a novel genegene
interaction finding). A number of secondary/exploratory hypotheses were rejected, of which the
most plausible finding include that the improvement in emotional disinhibition in the wild-type TT subjects of the FTO rs1421085 polymorphism was associated with a more pronounced decrease in BMI over the six
month weight loss period.
The integration of the results from this study with the literature indicates that there is insufficient evidence
at this stage for genetic screening of the polymorphisms investigated in this study and the provision of
evidence-based personalized recommendations for weight loss in obese individuals. It is recommended
that these associations should be viewed as priority in future research. / AFRIKAANSE OPSOMMING: Genetiese sifting om die resultate van vetsug behandeling te verbeter is beskikbaar ten spyte van ‘n tekort
aan genoegsame bewyse, spesifiek ten opsigte van Kaukasiërs van Suid-Afrika.
Die doel van hierdie studie was om die assosiasie tussen genotipe (sewe polimorfismes) en liggaamsmassa
indeks (LMI), gesondheid en lewenstyl indikatore in ‘n dwarssnit (cross-sectional) steekproef van
oorgewig/vetsugtige Kaukasiër volwassenes (n=133) te ondersoek, asook die assosiasie tussen genotipe en
gewigsverlies uitkomste na afloop van ‘n intervensie (n=88) in ‘n kwasi-eksperimentele studie ontwerp (tydreeks).
Die intervensie het bestaan uit ‘n 24-week konserwatiewe gewigsverlies program met dieet, fisieke
aktiwiteit en gedragskomponente.
Die primêre nul hipotese vir die dwarsnit steekproef, naamlik dat daar geen assosiasie tussen genotipe en
LMI is nie, is nie verwerp nie. ‘n Aantal sekondêre/spekulatiewe hipotesis is verwerp waarvan die mees
geloofwaardige assosiasies (gebasseer op ondersteuning van die literatuur en ‘n fisiologiese basis vir die
bevinding) die volgende insluit: 1) die mutante TT homosigote van die GNB3 C825T polimorfisme het
moontlik ‘n hoër risiko vir die ontwikkeling van die metaboliese sindroom (MetS) aangesien hulle
betekenisvolle hoër vastende trigliseriede en glukose vlakke gehad het, ‘n grooter aantal kenmerke gehad
het wat aan die diagnostiese afsnykriteria vir MetS voldoen en ‘n grooter aantal van hierdie persone was
met MetS gediagnoseer in vergelyking met die wilde-tipe C-alleel draers; en 2) persone met die mutante
allele van die FTO rs1421085 of rs17817449 polimorfismes het moontlik ‘n swakker eetgedrag (‘n hoër
rigiede kontrole, gewoonte en emosionele disinhibisie, waarneembare honger en interne lokus van honger)
en ‘n hoër inname van hoë-vet voedsel.
Die primêre nul hipotese vir die intervensie steekproef, naamlik dat daar geen assosiasie tussen genotipe
en gewigsverlies uitkomste is nie, is nie vir die FABP2 Ala54Thr, INSIG2 rs7566605, FTO rs1421085, ADRB3
Trp64Arg en GNB3 C825T polimorfismes verwerp nie. Dit was egter in sommige gevalle vir die volgende
assosiasies verwerp: 1) Die wilde-tipe TT homosigote van die FTO rs17817449 polimorfisme het
betekenisvol meer gewig in die eerste twee maande van die program verloor in vergelyking met die
mutante alleel draers (dit is ‘n nuwe bevinding); 2) Die wilde-tipe Arg16Arg homosigote van die ADRB2
Arg16Gly polimorfisme het betekenisvol meer gewig gedurende die eerste maand van die program verloor
in vergelyking met die mutante alleel draers (hierdie bevinding word ondersteun deur een ander
intervensie studie); 3) Persone met ‘n mutante C-alleel van die INSIG2 rs7566605 polimorfisme en ‘n
mutante Gly16-allele van die ADRB2 Arg16Gly polimorfisme het minder gewig tydens die ses maande
intervensie periode verloor (dit is ‘n nuwe geen-geen interaksie bevinding). ‘n Aantal sekondêre/
spekulatiewe hipoteses is verwerp, waarvan die mees geloofwaardigste bevinding insluit dat ‘n verbetering in emosionele disinhibisie van die wild-tipe TT persone van die FTO rs1421085 polimorfisme geassosieer
was met ‘n meer prominente daling in LMI oor die ses maande gewigsverlies periode.
Die integrasie van die resultate van hierdie navorsing met die literatuur dui aan dat daar op hierdie stadium
onvoldoende bewyse vir genetiese sifting en die voorsiening van bewys-gebasseerde persoonlike
aanbevelings vir gewigsverlies in vetsugtig individue bestaan vir die polimorfismes wat ondersoek is. Dit
word aanbeveel dat hierdie assosiasies as prioriteit in toekomstige navorsing beskou moet word.
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Immune and satellite cells : important role players in muscle recovery after injuryKruger, Maria Jacoba 03 1900 (has links)
Thesis (PhD (Physiological Sciences))--University of Stellenbosch, 2011. / Includes bibliography. / ENGLISH ABSTRACT: Muscle injuries are associated with changes in skeletal muscle as well as the immune
system. All studies investigating possible treatment modalities have found both positive and
negative effects on muscle recovery. Since no universally accepted treatment modality
exists, this thesis aims to determine whether a plant-derived antioxidant, proanthocyanidolic
oligomer (PCO), might prove beneficial as treatment for sports injuries in order for athletes to
return to the sports field quicker. The difference in recovery of muscle following both chronic
(supplementation started 14 days prior to injury and continued thereafter) and acute
supplementation (supplementation started two hours after injury) were also investigated.
Both chronic and acute PCO supplementation in a rat hindlimb contusion injury model
resulted in earlier muscle recovery, verified by an earlier satellite cell response compared to
the placebo group. This effect was most prominent already at the four hour time point
following injury, compared to day seven and three after chronic and acute placebo treatment
respectively. PCO supplementation also resulted in quicker foetal myosin heavy chain
(MHCf) expression compared to placebo treatment. Chronic supplementation specifically
resulted in a blunted circulatory pro-inflammatory cytokine response, whilst allowing for a
significant increase in IL-10, an anti-inflammatory cytokine, on day three (in the PCO group
only). At tissue level, the response of the muscle pro-inflammatory cytokines, TNF- and IL-
6, coincided with the satellite cell response. Macrophage infiltration into the injured muscle
also followed a similar pattern to that seen for the pro-inflammatory cytokines. Macrophages
invaded the injured area quicker when supplemented with PCO chronically, however,
macrophage infiltration could not explain the cytokine response seen with acute
supplementation. Both chronic and acute supplementation with PCO was responsible for a
severely blunted neutrophil response, a novel finding of this particular antioxidant.
The main findings of the in vivo rodent study were that PCO was able to blunt the neutrophil
response, whilst allowing for earlier macrophage infiltration. To establish possible
mechanisms by which PCO might exert these beneficial effects, further analysis included determining macrophage phenotypes and neutrophil numbers in circulation. An in vitro
neutrophil migration assay was also employed to further elucidate PCO’s ability to blunt
neutrophil infiltration into the injured area. For this study, conditioned plasma were harvested
from experimental animals and added together with neutrophils from control rats and
granulocyte colony stimulating factor (G-CSF) to the insert of the migration chamber. A
chemotactic factor, N-formyl methionine-leucine-phenylalanine (fMLP), was added to the
bottom well and neutrophils were allowed to migrate for two hours. Results from this study
indicated that neutrophil migration was attenuated in vitro in the presence of conditioned
plasma from PCO supplemented rats only.
The studies in this thesis on the effect of PCO on parameters of muscle and the immune
system led to the following main conclusions: a) PCO supplementation resulted in earlier
muscle recovery as a result of earlier satellite cell activation and MHCf synthesis; b) PCO
favours an anti-inflammatory cytokine reaction, whilst blunting the pro-inflammatory cytokine
response; and c) PCO blunted the neutrophil response whilst facilitating earlier macrophage
infiltration into the injured area. The specific mechanism of action of PCO to blunt the
neutrophil response specifically, possibly includes the ability to suppress adhesion molecule
expression on the neutrophils themselves. However, this warrants further investigation. / AFRIKAANSE OPSOMMING: Spier beserings word geassosiëer met veranderinge in skeletspier sowel as die
immuunstelsel. Meeste studies wat moontlike behandelingsopsies ondersoek, het beide
positiewe en negatiewe spierherstel gerapporteer. Omrede daar geen universele
behandelingsmoontlikheid bestaan nie, is die doel van hierdie tesis om die effek van ‘n
plantgebaseerde anti-oksidant, pro-antosianiedoliese oligomeer (PSO), as ‘n voordelige
behandelingstrategie vir sportbeserings te toets. Die verskil in spierherstel na beide kroniese
(supplementering wat 14 dae voor besering begin is, en volgehou is daarna) en akute
supplementering (supplementering het twee uur na besering begin), is ook ondersoek.
Beide kroniese en akute PSO supplementering, in ‘n rot agterbeen-kneusbeseringmodel, het
gelei tot vroeë spierherstel. Die bevindinge is geverifiëer deur ‘n vroeë satelietselrespons in
vergelyking met die plasebo groep. Hierdie effek was reeds opvallend vier uur na besering,
in vergelyking met die dag sewe en dag drie tydpunt tydens kroniese en acute plasebo
behandeling onderskeidelik. In vergelyking met die kontrole groep, het PSO
supplementering ook gelei to vininger uitdrukking van miosienswaarketting (MHCf). Kroniese
supplementering het spesifiek gelei to ‘n onderdrukte sirkulatoriese pro-inflammatoriese
sitokien response, terwyl ‘n betekenisvolle toename in IL-10 op dag drie (in die PSO groep
alleenlik) waargeneem is.
Op weefselvlak, het die pro-inflammatoriese sitokiene, IL-6 en TNF- , dieselfde patron
gevolg as die van satelietselle. Makrofaaginfiltrasie binne die beseerde spier het ook ‘n
soorgelyke patroon gevolg. Makrofage het die beseerde area vinniger geïnfiltreer in die
kronies PSO-gesupplementeerde groep, maar kon nie die sitokienrespons, wat waargeneem
is met akute supplementasie, verklaar nie. Beide kroniese en akute PSO supplementering
was verantwoordelik vir ‘n onderdrukte neutrofiel respons, wat ‘n nuwe bevinding is vir
hierdie spesifieke anti-oksidant. Die hoof bevindinge in die in vivo rotstudies, is dat PSO instaat is om die neutrofielrespons te
onderdruk, en sodoende vroeë makrofaaginfiltrasie teweeg te bring. Om meganismes
waarby PSO hierdie voordelige effekte veroorsaak te ondersoek, is verdere analises gedoen
om makrofaagfenotipe en neutrofielgetalle in die sirkulasie te bepaal. ‘n In vitro
neutrofielmigrasie studie is ook aangewend om PSO se vermoë om neutrofielinfiltrasie in die
beseerde area te onderdruk, te ondersoek. Neutrofiele van kontrole rotte, tesame met
gekondisioneerde plasma van eksperimentele diere en granulosiet-kolonie stimulerende
faktor (G-KSF), is toegelaat om vir twee ure in die teenwoordigheid van ‘n chemotaktiese
faktor, N-formiel metionien-leusien-fenielalanien (fMLP) te migreer. Resultate van hierdie
studie het aangetoon dat neutrofielmigrasie, in vitro, alleenlik onderdruk word in die
teenwoordigheid van gekondisioneerde plasma van PSO-gesupplementeerde rotte.
Die studies in hierdie tesis oor die effek van PSO op parameters van spier en die
immuunsisteem, het tot die volgende hoofgevolgtrekkings gelei: a) PSO supplementering
het vroeë spierherstel, as gevolge van vroeë satelietselaktivering en MHCf sintese, teweeg
gebring; b) PSO verkies ‘n anti-inflammatoriese sitokien reaksie, terwyl dit die proinflammatoriese
sitokienrespons onderdruk; en c) PSO onderdruk die neutrofielrespons,
terwyl vroeë makrofaaginfiltrasie in die beseerde area gefasiliteer word. Die spesifieke
meganisme van aksie van PSO, om die neutrofielrespons te onderdruk, kan moontlik die
vermoë van neutrofiele om adhesie molekule uit te druk, insluit. Hierdie aanname moet egter
verder ondersoek word.
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