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IN VITRO INTERACTION OF MYCOBACTERIUM AVIUM WITH INTESTINAL EPITHELIAL CELLS.Mapother, Mary Elizabeth. January 1982 (has links)
No description available.
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The impact of the steroid hormones medroxyprogesterone acetate, cortisol and progesterone on protective immunity to tuberculosisKleynhans, Leanie 03 1900 (has links)
Thesis (PhD)--Stellenbosch University, 2012. / Bibliography / ENGLISH ABSTRACT: Most individuals latently infected with Mycobacterium tuberculosis (Mtb) contain the infection by a
balance of effector and regulatory immune responses. However, this balance can be influenced by
steroid hormones such as glucocorticoids (GCs), which are known to increase the risk of reactivation of
TB. The contraceptive medroxyprogesterone acetate (MPA), which also possesses selective
glucocorticoid activity, is widely used in developing countries with approximately 60% of women on
contraceptives using MPA in our study cohort. Therefore, our aim was to investigate the effect of this
hormone on protective immune responses to BCG in HIV negative household contacts of active TB
patients. When PBMCs of TB household contacts were stimulated with BCG in the presence of 10 μM
MPA; this hormone displayed both glucocorticoid as well as progestogenic properties. Similarly to
cortisol, MPA suppressed antigen specific expression of a range of cytokines including IL-1α, IL-1ra, IL-
17, TNFα, IL-5 and IFNγ. Dose response curves showed that MPA can also alter expression of some
cytokines at lower contraceptive doses (in the nano molar range). To assess whether this effect of MPA
in vitro also occurs in women using this hormone as contraceptive the PBMCs of MPA users and controls
were stimulated with BCG and the levels of up to 29 different cytokines measured by luminex analysis.
PBMCs of MPA users produced significantly lower levels of cytokines involved in immune responses
against Mtb such as IL-12p40, IL-1α, IL-10, IL-13 and G-CSF, which corresponds with lower numbers of
circulating monocytes observed in these women. These findings warrant further investigation and clinical
trials should investigate the risk of progression from latent to active TB disease in women using this
contraceptive. These trials, however, require a large number of participants and are prohibitively
expensive; therefore it was decided to setup an Mtb/MPA mouse model to determine the effect of MPA on
the disease outcome. BALB/c and C57BL/6 mice were injected with a weekly dose of one mg MPA or
PBS and infected with 30 colony forming units of Mtb H37Rv one week after commencing the hormonal
treatment. Both strains were included to establish which strain best represents the human model. Three
and eight weeks post infection the MPA treated C57BL/6 mice had a significantly higher bacterial load in
their lungs compared to untreated mice, whereas no difference was found in the bacterial loads of the
BALB/c mice. MPA treated C57BL/6 mice had significantly lower serum levels of IL-10 and G-CSF and
MPA treated BALB/c mice lower serum levels of IFNγ, when compared to untreated mice. Furthermore,
cells isolated from the MLNs of MPA treated C57BL/6 mice, produced significantly less TNFα, significantly
more IP-10 and less IL-10 in response to PPD, while MLN cells of MPA treated BALB/c mice produced
significantly less IFNγ, IL-2, IL-17, GM-CSF and MCP-1. Data of the C57BL/6 mouse strain correlated
with our human data and can it therefore be said that the C57BL/6 mouse strain, together with the serum
concentration of MPA used in these experiments, is a good model to determine the effect of MPA in the
context of a low dose Mtb infection. To conclude MPA use could therefore alter susceptibility to TB, TB
disease severity as well as change the efficacy of new BCG-based vaccines, especially prime-boost
vaccine strategies which may be administered to adult of adolescent women in the future. / AFRIKAANSE OPSOMMING: Die meeste mense wat latent met Mycobacterium tuberculosis (Mtb) geïnfekteer is, hou die infeksie onder
beheer deur ʼn balans te handhaaf tussen effektor en regulatoriese immuunresponse. Hierdie balans kan
egter beïnvloed word deur steroïedhormone soos glukokortikoïede (GCs), wat bewys is om die risiko van
die heraktivering van TB te verhoog. Die voorbehoedmiddel medroksiprogesteroon-asetaat (MPA), wat
ook selektiewe glukokortikoïed-aktiwiteit toon, word wyd gebruik in ontwikkelende lande en omtrent 60%
van die vrouens in ons studie-bevolking wat voorbehoedmiddels gebruik, gebruik MPA. Om dié rede wou
ons die effek van hierdie hormoon op die beskermende immuun-response teenoor M.bovis Bacilli
Calmette-Guérin (BCG) in HIV negatiewe huishoudelike kontakte (HHKe) van pasiënte met aktiewe TB
ondersoek. Ons het gevind dat wanneer perifere bloed mononukleêre selle (PBMSe) met BCG
gestimuleer word in die teenwoordigheid van 10 μM MPA, hierdie hormoon beide glukokortikoïede en
progesterogeniese eienskappe toon. Soos kortisol het MPA die antigeenspesifieke-uitdrukking van ʼn
reeks sitokiene, insluitend IL-1α, IL-1ra, IL-17, TNFα, IL-5 en IFNγ, onderdruk. Respons kurwes wat
verskillende konsentrasies van hormoon insluit, het getoon dat MPA ook by laer (nano-molare) dosisse
die uitdrukking van sommige sitokiene kon verander. Om te bepaal of hierdie in vitro effek van MPA ook
in vrouens wat MPA as voorbehoedmiddel gebruik voorkom, het ons PBMSe van MPA-gebruikers and
kontroles met BCG gestimuleer en die vlakke van tot 29 verskillende sitokiene met behulp van Luminexanalise
gemeet. PBMSe van MPA-gebruikers produseer beduidende laer vlakke van IL-12p40, IL-1α, IL-
10, IL-13 en G-CSF, wat elk in imuunafweerreaksies teen Mtb betrokke is. Die afname in dié sitokiene
het gepaard gegaan met laer hoeveelhede sirkulerende monosiete. Ons resultate regverdig verdere
ondersoeke en kliniese proewe behoort die risiko van progressie vanaf latente tot aktiewe TB in vrouens
wat hierdie voorbehoedmiddel gebruik te bepaal. Sulke proewe vereis egter groot getalle deelnemers en
is skrikwekkend duur, om die rede het ons besluit om ʼn Mtb/MPA muis-model op te stel om sodoende die
algehele effek van MPA op die uitkoms van die siekte te bepaal. BALB/c en C57BL/6 muise is met ʼn
weeklikse dosis van een mg MPA of sout oplossing ingespuit en een week na die aanvang van die
hormoon behandeling met 30 kolonie-vormende eenhede Mtb H37Rv geïnfekteer. Beide muis tipes was
ingesluit om sodoende te bepaal watter tipe die mens data die beste verteenwoordig. Drie en agt weke
na die infeksie het die MPA-behandelde C57BL/6 muise ‘n beduidende hoër bakteriële lading in hul longe
gehad as die onbehandelde muise, maar was daar geen verskil in die bakteriële ladings in die longe van
die BALB/c muise nie. MPA-behandelde C57BL/6 muise het beduidende laer serumvlakke van IL-10 en
G-CSF gehad, terwyl MPA-behandelde BALB/c muise laer serumvlakke van IFNγ gehad het. Verder het
ons gevind dat die geisoleerde limfosiete van MPA-behandelde C57BL/6 muise beduidend minder TNFα,
beduidend meer IP-10 en minder IL-10 geproduseer het na stimulasie met PPD, terwyl die limfosiete van
MPA-behandelde BALB/c muise beduidend minder IFNγ, IL-2, IL-17, GM-CSF en MCP-1 geproduseer
het. Data van die C57BL/6 muise stem ooreen met die van ons mens studie en ons kan dus vermeld dat
die C57BL/6 muise, tesame met die spesifieke serumkonsentrasie van MPA wat gebruik is, ʼn goeie
model is om die effek van MPA in die konteks van ʼn lae-dosis Mtb-infeksie te bestudeer. MPA gebruik
kan dus die vatbaarheid vir TB, asook die erns van die siekte verander en kan ook die effektiwiteit van
nuwe BCG-gebaseerde entstowwe, veral prima-hupstoot enstowwe, wat moontlik in die nabye toekoms
vir volwasse en adolessente vroue toegedien kan word, verander.
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Distinct immune profiles of recently exposed household contacts in a tuberculosis endemic setting in the Western CapeNgombane, Nokwanda Crystal 03 1900 (has links)
Thesis (MScMedSc)--University of Stellenbosch, 2011. / Please refer to full text to view abstract.
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