Analysis of genetic variants in the 5' regulatory region of the ALAS1 gene in South African patients with variegate porphyria (VP) /

Du Plessis, Nelita.

January 2007

Thesis (MSc)--University of Stellenbosch, 2007. / Bibliography. Also available via the Internet.

Porphyria

Mutation analysis of four genes implicated in iron homeostasis in porphyria cutanea tarda (PCT) patients /

Panton, Nicola.

January 2008

Thesis (MSc)--University of Stellenbosch, 2008. / Bibliography. Also available via the Internet.

Porphyria

Biochemical studies in drug-induced porphyrias in the rat : with a review of the literature on experimental porphyria and an investigation of thirteen human cases

Ginsburg, Aubrey David

06 April 2020

The group of disorders characterized by disturbances of porphyrin metabolism pose .many fascinating problems. The drug-induced porphyrias in animals provide a model whereby these problems may be investigated by techniques which cannot be applied to man. The consumption of alcoholic beverages or other chemical substances has been associated with the development of porphyrinuria and porphyria, but it is controversial whether these agents are of primary aetiological importance. or 'Whether they precipitate the· disease in genetically predisposed individuals. The Turkish epidemic of porphyrla has shown conclusively·that this disease may occur as an acquired condition in man. and a variety of compounds has been shown to be capable of inducing porphyria in animals.

porphyria

Observations on drug-induced porphyria : with espescial reference to the role of ribonucleic acid

Hickman, Rosemary

01 August 2017

No description available.

Porphyria

Porphyria - Aetiology

Studies on [delta]-aminolaevulinic acid synthetase induced in guinea pig liver by 3,5-dicarbethoxy-1,4-dihydrocollidine

Irving, Elizabeth Anne

January 1969

xvii, 179 leaves : ill., appendices / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Thesis (Ph.D.)--University of Adelaide, Dept. of Biochemistry, 1970

Enzymes.

Porphyria.

Studies on [delta]-aminolaevulinic acid synthetase induced in guinea pig liver by 3,5-dicarbethoxy-1,4-dihydrocollidine.

Irving, Elizabeth Anne.

January 1969

Thesis (Ph.D.) -- University of Adelaide, Dept. of Biochemistry, 1970.

Enzymes. Porphyria.

Investigation of the possible influences of candidate modifier genes on the clinical expression of variegate porphyria (VP)

Steyn, Ilse

12 1900

Thesis (MSc)--University of Stellenbosch, 2002. / ENGLISH ABSTRACT: Variegate porphyria (VP, MIM 176200) is a low penetrance autosomal dominant disorder that stems from mutations in the protoporphyrinogen oxidase (PPOX) gene. VP is found in most populations, but has a high prevalence in the South African Afrikaner population with most patients inheriting the same PPOX mutation (R59W) from a common ancestor. The clinical manifestations of the disease include acute neurovisceral attacks and/or cutaneous photosensitivity. Great variation in the clinical presentation of VP is observed; even in members of the same family that share a common genetic background and that have been exposed to similar environmental factors. Candidate genes that may have an influence on phenotypic variation due to the regulatory function in the haem biosynthetic pathway include the two deltaaminolevulinic acid synthase (ALAS) genes and the porphobilinogen deaminase (PBGD) gene. Sequence homology searches between different species indicated that the ALAS-1, ALAS-2 and PBGD genes are highly conserved, indicating that these genes have an important function to fulfill in the haem biosynthetic pathway. The study population of 25 R59W individuals were divided in four categories according to their clinical presentation. The distribution of clinical symptoms observed in this study corresponds with results from previous studies. Conformation sensitive gel electrophoresis (CSGE), conventional single stranded conformation polymorphism analysis (SSCP) and two buffer SSCP analysis were implemented to screen for possible sequence variants. The exons of all three genes as well as the adjacent intronic sequences were investigated. A total of six sequence variation sites were identified of which five had previously been described single nucleotide polymorphisms (ALAS-1: 4713 T>C; PBGD: -64 C>T, 3581 A>G, 6479 G>T, 7064 C>A)] and a novel 8bp deletion (PBGD: 4582_ 4589del). No sequence variant was identified in the ALAS-2 gene. The CSGE method proved to have the highest sensitivity (83%), identifying five of six sequence variant sites. The conventional SSCP method identified only three (50%) sequence variant sites, while the two buffer system detected two (33%) of the sequence variants. The 4713 T>C SNP in exon 4 of the ALAS-1 gene and the -64 C>T SNP in the PBGD gene were selected for further investigation due to their location in the respective genes. These sequence variants were typed in 50 patients and 50 control subjects matched for ethnic background. The relationship between variation at these loci and clinical features was investigated. No statistical significant association was observed for either of the 4713 T>C SNP (P= 0.717) or the -64 C>T SNP (P= 0.931). Genetic modifying factors make a variable contribution to the total clinical picture and are difficult to identify in small populations. Due to the fact that we only had a limited number of VP samples, association cannot be ruled out. This study does, however, provide insight into investigational approaches that should be undertaken in future research concerning the ALAS and PBGD genes. Further knowledge concerning the haem biosynthetic pathway could ultimately lead to the understanding and assessment of the clinical expression observed in individuals with VP. / AFRIKAANSE OPSOMMING: Variegate porfirie (VP, MIM 176200) is 'n lae penetrasie outosomaal dominante siekte wat veroorsaak word deur mutasies in die protoporfirienogeen oksidase (PPOX) geen. VP word gevind in die meeste populasies, maar het 'n hoë voorkoms in die Suid- Afrikaanse populasie waar meeste pasiente dieselfde PPOX mutasie (R59W) van 'n gemeenskaplike voorouer oorgeërf het. VP word gekenmerk deur akute neuroviserale aanvalle en/of fotosensitiewe vel. Groot variasie word egter waargeneem in die kliniese uitdrukking van VP, selfs in lede van dieselfde familie wat 'n gemeenskaplike genetiese agtergrond deel en wat blootgestel is aan dieselfde omgewingsfaktore. Kandidaat gene wat as gevolg van hulle regulatoriese funksie in die heem biosintetiese padweg 'n effek op die ekspressie van VP mag hê, sluit in die twee deltaaminolevuliniese suur sintase (ALAS) en die porfobilinogeen deaminase (PBGD) gene. Homologie ondersoeke van die ALAS-1, ALAS-2 en PBGD gene in verskillende spesies dui daarop dat die gene hoogs gekonserveerd is en dus gevolglik 'n belangrike funksie in die heem biosintetiese padweg vertolk. Die studie populasie van 25 R59W individue is verdeel in vier kategorieë op grond van hulle kliniese simptome. Die verspreiding van die kliniese simptome wat waargeneem is tydens hierdie studie stem ooreen met die resultate van vorige studies. Konformasie sensitiewe gel elektroforese (CSGE), konvensionele enkelstring konformasie polimorfisme analise (SSCP) en twee buffer SSCP analise is gebruik vir die identifisering van genetiese variasie. Die eksons van al drie gene, sowel as die aangrensende intron volgordes, is ondersoek. 'n Totaal van ses areas van genetiese variasie is geïdentifiseer, waarvan vyf reeds beskryfde polimorfismes is (ALAS-1: 4713 T>C; PBGD: -64 C>T, 3581 A>G, 6479 G>T, 7064 C>A) en 'n nuwe 8bp delesie (PBGD: 4582_ 4589del). Geen genetiese volgorde variasie is gevind in die ALAS-2 geen nie. Die CSGE metode het die hoogste sensitiwiteit getoon (83%) en het vyf van die ses volgorde variasies geïdentifiseer. Die konvensionele SSCP metode het slegs drie volgorde variasies geïdentifiseer (50%), terwyl die twee buffer deteksie-sisteem twee variasies geïdentifiseer (33%) het. Die 4713 T>C polimorfisme in ekson 4 van die ALAS-1 geen en die -64 C>T polimorfisme in die PBGD geen, is geselekteer vir verdere ondersoek as gevolg van hulle posisie in die respektiewe gene. Die volgorde variasies is getipeer in 50 R59W pasiënte sowel as in 'n kontrole groep van 50 individue met dieselfde etniese agtergrond. Die verband tussen die variasie by die lokusse en die kliniese kenmerke is ondersoek. Geen statisties beduidende assosiasie is waargeneem vir hetsy die 4713 T>C SNP (P= 0.717) of die -64 C>T SNP (P= 0.931). Genetiese modifiserende faktore word moeilik geïdentifiseer in klein populasies omdat hulle afsonderlike bydra tot die geheelbeeld van die kliniese simptome so varieerbaar is. 'n Relatiewe klein groep van VP pasiënte was tydens die studie beskikbaar en dus kan assosiasie nie uitgesluit word nie. Die studie verskaf egter insig in verband met toekomstige benaderings wat volg kan word in verdere ondersoeke van die ALAS en PBGD gene. Verdere kennis in verband met die heem biosihtetiese padweg kan uiteiHdelik lei tot die verduideliking en assesering van die kliHiese uitdrukking in vI=' individue.

Porphyria -- Genetic aspects

The Chester porphyria

Church, S.

January 1986

No description available.

610

Porphyria in the Chester area

Studies of the pathogenesis and treatment of acute intermittent porphyria

Herrick, Ariane L.

January 1989

The thesis examines the pathogenesis and treatment of acute intermittent porphyria (AIP), an inherited disorder of haem biosynthesis characterised biochemically by overproduction and increased excretion of porphyrin precursors, and clinically by neurovisceral crises which can be life-threatening. Both prevention and treatment of porphyric crises are considered. Acute attacks can be triggered by either endogenous or exogenous precipitants. A trial of hormonal suppression, using the luteinizing hormone releasing hormone analogue buserelin, in 7 patients suffering premenstrual attacks of AIP, suggested a trend towards clinical improvement on buserelin although response to treatment varied widely between patients. The relationship between endogenous steroids and disease activity in AIP was further examined by measuring urinary steroid metabolite excretion in patients with active, latent, and quiescent disease. In patients with active AIP the ratio of 5α to 5β urinary steroid metabolites was reduced, as was total steroid metabolite excretion. The finding of elevated plasma sex hormone-binding globulin concentrations in patients with active AIP is also reported. Drug porphyrinogenicity is discussed with reference to antidepressants and anticonvulsants. Preliminary anecdotal experience of the use of the haem derivative haem arginate in the treatment of 37 acute attacks of porphyria is described, and the first double-blind controlled trial of haem derivative treatment reported. This studied 21 attacks in 12 patients. While haem arginate invariably produced a marked fall in porphyrin precursor excretion, it did not significantly affect clinical outcome, although there was a trend in favour of haem treatment. In 7 attacks of AIP, haem arginate corrected the impaired hepatic mixed function oxygenase activity which is a recognised feature of AIP : antipyrine clearance was increased. The finding of raised blood lactate levels after glucose loading suggested that cytochrome deficiency affecting the terminal respiratory chain also occurs in AIP. It is postulated that the genetic, metabolic, endocrine and hepatic abnormalities of AIP may be inter-related through haem deficiency.

610

Porphyria treatment

Studies on porphyria as an indicator of polyhalogenated aromatic hydrocarbon exposure.

Kennedy, Sean W. (Sean William), Carleton University. Dissertation. Chemistry.

January 1988

Thesis (Ph. D.)--Carleton University, 1988. / Also available in electronic format on the Internet.