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The design, development and testing of a non-invasive continuous crystalliser system for the study of calcium oxalate crystallisation processes

Includes bibliographies.

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Main Author: Bretherton, Tracy Ann
Other Authors: Rodgers, Allen L
Format: Thesis
Language:English
Published: Department of Chemistry 2016
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access_status_str Open Access
author Bretherton, Tracy Ann
author2 Rodgers, Allen L
author_browse Bretherton, Tracy Ann
Rodgers, Allen L
author_facet Rodgers, Allen L
Bretherton, Tracy Ann
author_sort Bretherton, Tracy Ann
collection Thesis
description Includes bibliographies.
format Thesis
id oai:open.uct.ac.za:11427/16137
institution University of Cape Town (South Africa)
language eng
last_indexed 2026-06-10T12:34:39.560Z
license_str Not specified — see source repository
provenance_str_mv Harvested via OAI-PMH from UCTD — University of Cape Town Open Access Repository
publishDate 2016
publishDateRange 2016
publishDateSort 2016
publisher Department of Chemistry
publisherStr Department of Chemistry
record_format dspace
source_str UCTD — University of Cape Town Open Access Repository
spelling oai:open.uct.ac.za:11427/16137 The design, development and testing of a non-invasive continuous crystalliser system for the study of calcium oxalate crystallisation processes Bretherton, Tracy Ann Rodgers, Allen L Chemistry Includes bibliographies. The MSMPR was designed according to chemical engineering principles and tests showed that it conforms to the assumptions necessary for conventional MSMPR analysis. Various crystalliser offtakes and six system designs were developed and tested to allow measurements using the thermostatted flow cell. The flow cell allows for continuous measurement of the sample dispersion using a noninvasive monitoring instrument - a Malvern Particle Size Analyser. In this technique, measurement of the steady state crystal size distribution is based on a diffraction pattern produced by the particles in a parallel beam of monochromatic light. Comparative measurements were obtained by sampling directly from the crystalliser and analysing the product in a Coulter Counter. In this technique, the steady state crystal size distribution is measured by the change in resistance as particles, in an electrically conductive liquid, pass through the Coulter aperture. Due to the large volumes required by the crystalliser, it was necessary to pool urines. Aliquots of volume 1. 5 dm3 from the 24 hour urines of each of 8 male controls were pooled. The first series of experiments were performed to investigate the effect on calcium oxalate crystallisation of varying the concentration of sodium oxalate solutions used to initiate crystallisation, and also to investigate the effect of varying the temperature. A further series of experiments was performed to determine the effect of adding inhibitors individually (citrate, magnesium, chondroitin sulphate A) and in combination (citrate and magnesium). The inhibitor experiments were performed using two different approaches. In the first, the pooled urine was pre-treated with the inhibitor prior to being introduced into the crystalliser. In the second set of experiments, the inhibitor was introduced into the crystalliser via a separate, independent feed. It is suggested that these approaches represent crude models respectively of (a) the endogenous presence of inhibitors and (b) the oral administration of such inhibitors. Each individual experiment was performed using three different urine pools. The steady state crystal size distributions obtained from both the Coulter and the Malvern instruments were used to determine nucleation and growth rates in each urine. Scanning electron microscopy was used to obtain qualitative and semi-quantitative data related to crystal morphology, number, size and degree of aggregation. Both nucleation and growth rates increased as the concentrations of the initiating sodium oxalate solutions increased. Nucleation and growth rates also increased with increasing temperatures. In the latter series of experiments, different calcium oxalate crystal phases precipitated at the various temperatures. Citrate inhibited nucleation and growth of calcium oxalate, irrespective of how it was admitted to the crystalliser. Magnesium was found to inhibit growth only and, like citrate, this role was independent of how it was introduced into the crystalliser. Although both inhibited growth, the effect of the citrate was greater. When both components were added in combination, inhibition was observed to be additive. In all cases, inhibitory effects increased with increasing concentration. Chondroitin sulphate A was found to inhibit nucleation; inhibition of growth was minimal at the concentrations tested. Aggregation of calcium oxalate crystals was found to be inhibited by chondroitin sulphate A. The results of the calcium oxalate crystallisation kinetic studies, obtained by using Malvern particle sizing and Coulter Counter techniques independently of each other, showed general agreement. These results, in turn, were in agreement with the published results of others, thereby lending confidence to the findings and highlighting the potential application of the non-invasive continuous crystalliser in urolithiasis research. 2016-01-02T04:52:04Z 2016-01-02T04:52:04Z 1996 Doctoral Thesis Doctoral PhD http://hdl.handle.net/11427/16137 eng application/pdf Department of Chemistry Faculty of Science University of Cape Town
spellingShingle Chemistry
Bretherton, Tracy Ann
The design, development and testing of a non-invasive continuous crystalliser system for the study of calcium oxalate crystallisation processes
thesis_degree_str Doctoral
title The design, development and testing of a non-invasive continuous crystalliser system for the study of calcium oxalate crystallisation processes
title_full The design, development and testing of a non-invasive continuous crystalliser system for the study of calcium oxalate crystallisation processes
title_fullStr The design, development and testing of a non-invasive continuous crystalliser system for the study of calcium oxalate crystallisation processes
title_full_unstemmed The design, development and testing of a non-invasive continuous crystalliser system for the study of calcium oxalate crystallisation processes
title_short The design, development and testing of a non-invasive continuous crystalliser system for the study of calcium oxalate crystallisation processes
title_sort design development and testing of a non invasive continuous crystalliser system for the study of calcium oxalate crystallisation processes
topic Chemistry
url http://hdl.handle.net/11427/16137
work_keys_str_mv AT brethertontracyann thedesigndevelopmentandtestingofanoninvasivecontinuouscrystallisersystemforthestudyofcalciumoxalatecrystallisationprocesses
AT brethertontracyann designdevelopmentandtestingofanoninvasivecontinuouscrystallisersystemforthestudyofcalciumoxalatecrystallisationprocesses