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Dive into the research topics where Frans Maritz is active.

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Featured researches published by Frans Maritz.


Thorax | 1995

Use of adenosine deaminase as a diagnostic tool for tuberculous pleurisy.

Lesley J. Burgess; Frans Maritz; I. Le Roux; J. J. F. Taljaard

BACKGROUND--A statistical audit of adenosine deaminase (ADA) in pleural effusions was undertaken. METHODS--ADA analysis, cytological and microbiological examinations, and differential cell counts were performed on 462 pleural fluid samples. RESULTS--ADA activity in tuberculous effusions was higher than in any other diagnostic group. At a level of 50 U/l the sensitivity and specificity for the identification of tuberculosis was 90% and 89%, respectively. CONCLUSIONS--ADA activity remains a useful test in the evaluation of pleural effusions.


South African Medical Journal | 2008

Mortality in patients treated for tuberculous pericarditis in sub-Saharan Africa

Bongani M. Mayosi; Charles Shey Wiysonge; Mpiko Ntsekhe; Freedom Gumedze; Jimmy Volmink; Gary Maartens; Baby Thomas; Kandathil M Thomas; Abolade A. Awotedu; Bongani Thembela; Phindile Mntla; Frans Maritz; Duquesne C Nkouonlack; Vanessa Burch; Kevin Rebe; Andy Parrish; Karen Sliwa; Brian Z Vezi; Nowshad Alam; Basil G Brown; Trevor Gould; Tim Visser; Nombulelo P. Magula; Patrick Commerford

OBJECTIVE To determine the mortality rate and its predictors in patients with a presumptive diagnosis of tuberculous pericarditis in sub-Saharan Africa. DESIGN Between 1 March 2004 and 31 October 2004, we enrolled 185 consecutive patients with presumed tuberculous pericarditis from 15 referral hospitals in Cameroon, Nigeria and South Africa, and observed them during the 6-month course of antituberculosis treatment for the major outcome of mortality. This was an observational study, with the diagnosis and management of each patient left at the discretion of the attending physician. Using Cox regression, we have assessed the effect of clinical and therapeutic characteristics (recorded at baseline) on mortality during follow-up. RESULTS We obtained the vital status of 174 (94%) patients (median age 33; range 14 - 87 years). The overall mortality rate was 26%. Mortality was higher in patients who had clinical features of HIV infection than in those who did not (40% v. 17%, p=0.001). Independent predictors of death during followup were: (i) a proven non-tuberculosis final diagnosis (hazard ratio (HR) 5.35, 95% confidence interval (CI) 1.76 - 16.25), (ii) the presence of clinical signs of HIV infection (HR 2.28, CI 1.14 - 4.56), (iii) coexistent pulmonary tuberculosis (HR 2.33, CI 1.20 - 4.54), and (iv) older age (HR 1.02, CI 1.01 - 1.05). There was also a trend towards an increase in death rate in patients with haemodynamic instability (HR 1.80, CI 0.90 - 3.58) and a decrease in those who underwent pericardiocentesis (HR 0.34, CI 0.10 - 1.19). CONCLUSION A presumptive diagnosis of tuberculous pericarditis is associated with a high mortality in sub-Saharan Africa. Attention to rapid aetiological diagnosis of pericardial effusion and treatment of concomitant HIV infection may reduce the high mortality associated with the disease.


BMC Infectious Diseases | 2006

Clinical characteristics and initial management of patients with tuberculous pericarditis in the HIV era: the Investigation of the Management of Pericarditis in Africa (IMPI Africa) registry

Bongani M. Mayosi; Charles Shey Wiysonge; Mpiko Ntsekhe; Jimmy Volmink; Freedom Gumedze; Gary Maartens; Akinyemi Aje; Baby Thomas; Kandathil M Thomas; Abolade A. Awotedu; Bongani Thembela; Phindile Mntla; Frans Maritz; Kathleen Ngu Blackett; Duquesne C Nkouonlack; Vanessa Burch; Kevin Rebe; Andy Parish; Karen Sliwa; Brian Z Vezi; Nowshad Alam; Basil G Brown; Trevor Gould; Tim Visser; Muki Shey; Nombulelo P. Magula; Patrick Commerford

BackgroundThe incidence of tuberculous pericarditis has increased in Africa as a result of the human immunodeficiency virus (HIV) epidemic. However, the effect of HIV co-infection on clinical features and prognosis in tuberculous pericarditis is not well characterised. We have used baseline data of the Investigation of the Management of Pericarditis in Africa (IMPI Africa) registry to assess the impact of HIV co-infection on clinical presentation, diagnostic evaluation, and treatment of patients with suspected tuberculous pericarditis in sub-Saharan Africa.MethodsConsecutive adult patients in 15 hospitals in three countries in sub-Saharan Africa were recruited on commencement of treatment for tuberculous pericarditis, following informed consent. We recorded demographic, clinical, diagnostic and therapeutic information at baseline, and have used the chi-square test and analysis of variance to assess probabilities of significant differences (in these variables) between groups defined by HIV status.ResultsA total of 185 patients were enrolled from 01 March 2004 to 31 October 2004, 147 (79.5%) of whom had effusive, 28 (15.1%) effusive-constrictive, and 10 (5.4%) constrictive or acute dry pericarditis. Seventy-four (40%) had clinical features of HIV infection. Patients with clinical HIV disease were more likely to present with dyspnoea (odds ratio [OR] 3.2, 95% confidence interval [CI] 1.4 to 7.4, P = 0.005) and electrocardiographic features of myopericarditis (OR 2.8, 95% CI 1.1 to 6.9, P = 0.03). In addition to electrocardiographic features of myopericarditis, a positive HIV serological status was associated with greater cardiomegaly (OR 3.89, 95% CI 1.34 to 11.32, P = 0.01) and haemodynamic instability (OR 9.68, 95% CI 2.09 to 44.80, P = 0.0008). However, stage of pericardial disease at diagnosis and use of diagnostic tests were not related to clinical HIV status. Similar results were obtained for serological HIV status. Most patients were treated on clinical grounds, with microbiological evidence of tuberculosis obtained in only 13 (7.0%) patients. Adjunctive corticosteroids were used in 109 (58.9%) patients, with patients having clinical HIV disease less likely to be put on them (OR 0.37, 95% CI 0.20 to 0.68). Seven patients were on antiretroviral drugs.ConclusionPatients with suspected tuberculous pericarditis and HIV infection in Africa have greater evidence of myopericarditis, dyspnoea, and haemodynamic instability. These findings, if confirmed in other studies, may suggest more intensive management of the cardiac disease is warranted in patients with HIV-associated pericardial disease.


Clinical Genetics | 1999

Founder mutations in the LDL receptor gene contribute significantly to the familial hypercholesterolemia phenotype in the indigenous South African population of mixed ancestry

Odell Loubser; A. David Marais; Maritha J. Kotze; Nicole Godenir; Rochelle Thiart; Charlotte L. Scholtz; J. Nico P. de Villiers; Renate Hillermann; Jean C. Firth; Hellmuth Weich; Frans Maritz; Sheena Jones; Deneys R. van der Westhuyzen

The South African population harbors genes that are derived from varying degrees of admixture between indigenous groups and immigrants from Europe and the East. This study represents the first direct mutation‐based attempt to determine the impact of admixture from other gene pools on the familial hypercholesterolemia (FH) phenotype in the recently founded Coloured population of South Africa, a people of mixed ancestry. A cohort of 236 apparently unrelated patients with clinical features of FH was screened for a common mutation causing familial defective apolipoprotein B‐100 (FDB) and seven low‐density lipoprotein receptor (LDLR) gene defects known to be relatively common in South Africans with FH. Six founder‐type ‘South African mutations’ were responsible for FH in ∼20% of the study population, while only 1 patient tested positive for the familial defective apolipoprotein B‐100 mutation R3500Q. The detection of multiple founder‐type LDLR gene mutations originating from European, Indian and Jewish populations provides direct genetic evidence that Caucasoid admixture contributes significantly to the apparently high prevalence of FH in South African patients of mixed ancestry. This study contributes to our knowledge of the biological history of this unique population and illustrates the potential consequences of recent admixture in populations with different disease risks.


South African Medical Journal | 2004

Insulin resistance and vascular disease

Frans Maritz

The insulin resistance syndrome comprises a typical cluster of cardiovascular risk factors and is predicted to increase dramatically over the next few decades. The disease process starts many years before the condition is clinically obvious and targets primarily the cardiovascular system. The pathogenesis involves a complex interplay between all the associated cardiovascular risk factors but endothelial dysfunction plays a major role. Management of these patients involves management of all the associated risk factors and should be aimed primarily at early detection and the prevention of vascular morbidity and mortality in the short and long term.


Chest | 1996

Combined Use of Pleural Adenosine Deaminase With Lymphocyte/Neutrophil Ratio: Increased Specificity for the Diagnosis of Tuberculous Pleuritis

Lesley J. Burgess; Frans Maritz; Irene Le Roux; J.J. Frans Taljaard


Chest | 1995

Comparative Analysis of the Biochemical Parameters Used to Distinguish Between Pleural Transudates and Exudates

Lesley J. Burgess; Frans Maritz; J.J. Frans Taljaard


South African Medical Journal | 1982

Adenosine deaminase estimations in the differentiation of pleural effusions

Frans Maritz; C. Malan; I. M. Le Roux


Archive | 2012

Additional file 1

Bongani M. Mayosi; Charles Shey Wiysonge; Mpiko Ntsekhe; Jimmy Volmink; Freedom Gumedze; Gary Maartens; Akinyemi Aje; Baby Thomas; Kandathil M Thomas; Abolade A. Awotedu; Bongani Thembela; Phindile Mntla; Frans Maritz; Kathleen Ngu Blackett; Duquesne C Nkouonlack; Vanessa Burch; Kevin Rebe; Andy Parish; Karen Sliwa; Brian Z Vezi; Nowshad Alam; Basil G Brown; Trevor Gould; Tim Visser; Muki Shey; Nombulelo P. Magula; Patrick Commerford


South African Medical Journal | 1996

Flushes, night sweats and palpitations need to be treated seriously.

Lesley J. Burgess; Frans Maritz; Taljaard Jj

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Brian Z Vezi

University of KwaZulu-Natal

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Charles Shey Wiysonge

South African Medical Research Council

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Karen Sliwa

University of Cape Town

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Kevin Rebe

University of Cape Town

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