Determination of mercury chemical speciation in the presence of low molecular mass thiols and its importance for mercury methylation

Methylmercury (MeHg) is a neurotoxic compound that threatens the well-being of humans and wildlife. It is formed through the methylation of inorganic mercury (HgII) under suboxic/anoxic conditions in soils, sediment and waters. The chemical speciation of HgII, including specific HgII species in aque...

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Main Author: Liem-Nguyen, Van
Format: Doctoral Thesis
Language:English
Published: Umeå universitet, Kemiska institutionen 2016
Subjects:
ICP
Online Access:http://urn.kb.se/resolve?urn=urn:nbn:se:umu:diva-119938
http://nbn-resolving.de/urn:isbn:978-91-7601-469-1
id ndltd-UPSALLA1-oai-DiVA.org-umu-119938
record_format oai_dc
collection NDLTD
language English
format Doctoral Thesis
sources NDLTD
topic Mercury
methylmercury
LMM thiol
mass spectrometry
biogeochemistry
soil
sediment
ICP
WinSGW
modeling
S XANES
ligand exchange
stability constant
boreal wetlands
spellingShingle Mercury
methylmercury
LMM thiol
mass spectrometry
biogeochemistry
soil
sediment
ICP
WinSGW
modeling
S XANES
ligand exchange
stability constant
boreal wetlands
Liem-Nguyen, Van
Determination of mercury chemical speciation in the presence of low molecular mass thiols and its importance for mercury methylation
description Methylmercury (MeHg) is a neurotoxic compound that threatens the well-being of humans and wildlife. It is formed through the methylation of inorganic mercury (HgII) under suboxic/anoxic conditions in soils, sediment and waters. The chemical speciation of HgII, including specific HgII species in aqueous and solid/adsorbed phases, plays a key role in MeHg formation. Chemical forms of HgII which have been reported to be available for uptake in methylating bacteria include neutral HgII–sulfide complexes, HgII complexes with specific low molecular mass (LMM) thiols, and nanoparticulate HgS(s). Accurate determination of the chemical speciation of HgII is thus crucial when elucidating the mechanism of MeHg formation. The concentration of HgII–LMM thiols complexes is predicted to be extremely low (sub fM range). Current analytical methods do not allow direct quantification of HgII complexes due to the very low concentration of these complexes, and therefore determination rely on thermodynamic modeling. Accurate stability constants for HgII–LMM thiols complexes and quantification of LMM thiol ligands in environments are thus required to precisely determine the concentration of such complexes. In this thesis, a novel analytical method was developed based on online pre-concentration coupled with liquid chromatography tandem mass spectrometry to determine the concentration of 16 LMM thiols (Paper I). This method was successful in detecting 8 LMM thiols in boreal wetland porewaters, with mercaptoacetic acid and cysteine being the most abundant. The total concentration of individual detected LMM thiols ranged from sub nM (LOD=0.1 nM) to 77 nM. Moreover, the stability constant (β2) for HgII complexes with 15 LMM thiols were directly determined for the first time by competing ligand exchange experiments combined with liquid chromatography ICPMS analysis (Paper II). Values of log β2 for the reaction Hg2+ + 2LMM-RS- = Hg(LMM-RS)2 ranged from 34.6 for. Based on the determined constants of Hg(LMM-RS)2 complexes and state-of-the-art constants from literature for other HgII complexes, we established comprehensive thermodynamic speciation models for MeHg and HgII in boreal wetlands (Paper III). The speciation of HgII was coupled with the HgII methylation rate constant (km) determined with different enriched Hg isotope tracers (Paper IV). There was a good correlation (R2=0.88) between the km determined by a HgII(aq) tracer added as Hg(NO3)2 with high bioavailability and a tracer where HgII was bond to thiol groups in natural organic matter (HgII-NOM(ads)) and has a lower bioavailability. The HgII(aq) tracer was consistently methylated at 5 times higher rate than the HgII-NOM(ads) tracer. A good correlation was observed between the concentration of biologically produced LMM thiols and km in the boreal wetlands. In a mesocosm study of estuarine sediment-brackish water systems, increased concentration of phytoplankton chlorophyll α due to macro nutrient additions led to an increase in HgII methylation rate of the HgII(aq) but not of the HgII-NOM(ads) tracer or ambient HgII species (Paper V). Furthermore, simulated newly deposited HgII species from atmospheric and terrestrial sources were exhibited significantly higher HgII methylation rates when compared with simulated aged sediment HgII pools. Through the development and adoption of novel analytical methods, this thesis reveals the significance of LMM thiols in Hg biogeochemistry by precise determination of HgII–LMM thiol complexes in natural environmental systems.
author Liem-Nguyen, Van
author_facet Liem-Nguyen, Van
author_sort Liem-Nguyen, Van
title Determination of mercury chemical speciation in the presence of low molecular mass thiols and its importance for mercury methylation
title_short Determination of mercury chemical speciation in the presence of low molecular mass thiols and its importance for mercury methylation
title_full Determination of mercury chemical speciation in the presence of low molecular mass thiols and its importance for mercury methylation
title_fullStr Determination of mercury chemical speciation in the presence of low molecular mass thiols and its importance for mercury methylation
title_full_unstemmed Determination of mercury chemical speciation in the presence of low molecular mass thiols and its importance for mercury methylation
title_sort determination of mercury chemical speciation in the presence of low molecular mass thiols and its importance for mercury methylation
publisher Umeå universitet, Kemiska institutionen
publishDate 2016
url http://urn.kb.se/resolve?urn=urn:nbn:se:umu:diva-119938
http://nbn-resolving.de/urn:isbn:978-91-7601-469-1
work_keys_str_mv AT liemnguyenvan determinationofmercurychemicalspeciationinthepresenceoflowmolecularmassthiolsanditsimportanceformercurymethylation
_version_ 1718405552772481024
spelling ndltd-UPSALLA1-oai-DiVA.org-umu-1199382016-12-22T05:20:30ZDetermination of mercury chemical speciation in the presence of low molecular mass thiols and its importance for mercury methylationengLiem-Nguyen, VanUmeå universitet, Kemiska institutionenUmeå : Umeå universitet2016MercurymethylmercuryLMM thiolmass spectrometrybiogeochemistrysoilsedimentICPWinSGWmodelingS XANESligand exchangestability constantboreal wetlandsMethylmercury (MeHg) is a neurotoxic compound that threatens the well-being of humans and wildlife. It is formed through the methylation of inorganic mercury (HgII) under suboxic/anoxic conditions in soils, sediment and waters. The chemical speciation of HgII, including specific HgII species in aqueous and solid/adsorbed phases, plays a key role in MeHg formation. Chemical forms of HgII which have been reported to be available for uptake in methylating bacteria include neutral HgII–sulfide complexes, HgII complexes with specific low molecular mass (LMM) thiols, and nanoparticulate HgS(s). Accurate determination of the chemical speciation of HgII is thus crucial when elucidating the mechanism of MeHg formation. The concentration of HgII–LMM thiols complexes is predicted to be extremely low (sub fM range). Current analytical methods do not allow direct quantification of HgII complexes due to the very low concentration of these complexes, and therefore determination rely on thermodynamic modeling. Accurate stability constants for HgII–LMM thiols complexes and quantification of LMM thiol ligands in environments are thus required to precisely determine the concentration of such complexes. In this thesis, a novel analytical method was developed based on online pre-concentration coupled with liquid chromatography tandem mass spectrometry to determine the concentration of 16 LMM thiols (Paper I). This method was successful in detecting 8 LMM thiols in boreal wetland porewaters, with mercaptoacetic acid and cysteine being the most abundant. The total concentration of individual detected LMM thiols ranged from sub nM (LOD=0.1 nM) to 77 nM. Moreover, the stability constant (β2) for HgII complexes with 15 LMM thiols were directly determined for the first time by competing ligand exchange experiments combined with liquid chromatography ICPMS analysis (Paper II). Values of log β2 for the reaction Hg2+ + 2LMM-RS- = Hg(LMM-RS)2 ranged from 34.6 for. Based on the determined constants of Hg(LMM-RS)2 complexes and state-of-the-art constants from literature for other HgII complexes, we established comprehensive thermodynamic speciation models for MeHg and HgII in boreal wetlands (Paper III). The speciation of HgII was coupled with the HgII methylation rate constant (km) determined with different enriched Hg isotope tracers (Paper IV). There was a good correlation (R2=0.88) between the km determined by a HgII(aq) tracer added as Hg(NO3)2 with high bioavailability and a tracer where HgII was bond to thiol groups in natural organic matter (HgII-NOM(ads)) and has a lower bioavailability. The HgII(aq) tracer was consistently methylated at 5 times higher rate than the HgII-NOM(ads) tracer. A good correlation was observed between the concentration of biologically produced LMM thiols and km in the boreal wetlands. In a mesocosm study of estuarine sediment-brackish water systems, increased concentration of phytoplankton chlorophyll α due to macro nutrient additions led to an increase in HgII methylation rate of the HgII(aq) but not of the HgII-NOM(ads) tracer or ambient HgII species (Paper V). Furthermore, simulated newly deposited HgII species from atmospheric and terrestrial sources were exhibited significantly higher HgII methylation rates when compared with simulated aged sediment HgII pools. Through the development and adoption of novel analytical methods, this thesis reveals the significance of LMM thiols in Hg biogeochemistry by precise determination of HgII–LMM thiol complexes in natural environmental systems. Doctoral thesis, comprehensive summaryinfo:eu-repo/semantics/doctoralThesistexthttp://urn.kb.se/resolve?urn=urn:nbn:se:umu:diva-119938urn:isbn:978-91-7601-469-1application/pdfinfo:eu-repo/semantics/openAccess