Characterization of pyrene degradation by Mycobacterium sp. strain S65

Sho, Michiei, 1976-

January 2002

No description available.

Soil remediation.

Mycobacterium.

Bioremediation.

Pyrene (Chemical) -- Biodegradation.

ALTERED GENE EXPRESSION: A MECHANISM OF REPRODUCTIVE TOXICITY IN ZEBRAFISH (DANIO RERIO) EXPOSED TO BENZO[a]PYRENE

Hoffmann, Jennifer

19 August 2004

No description available.

Zebrafish

Benzo[a]pyrene

ovary

steroidogenic enzymes

mRNA

Pyrene degradation of biofilm-forming Paracoccus sp. DG25 isolated from oil polluted samples collected in petroleum storage Duc Giang, Hanoi / Khả năng phân hủy pyrene của chủng Paracoccus sp. DG25 phân lập từ các mẫu nhiễm dầu lấy tại kho xăng Đức Giang, Hà Nội

Le, Thi Nhi Cong, Cung, Thi Ngoc Mai, Vu, Thi Thanh, Nghiem, Ngoc Minh, Hoang, Phuong Ha, Do, Thi Lien, Do, Thi To Uyen

09 December 2015

In this study, a well biofilm-forming bacterial strain was isolated from oil contaminated water and sediment samples collected in petroleum storage Duc Giang, Hanoi. It was identified as Paracoccus sp. DG25 and registered in the GenBank database with the accession numbers KJ608354. Several biophysical and bio-chemical conditions for the biofilm formation of the strain were estimated such as pH, temperature, carbon sources and nitrogen sources. As the results the biofilm forming capacity was highest at pH 7, 37 oC, on maltose and supplemented with KNO3. Using these optimal conditions, the formed biofilm degraded 76.07 % of pyrene after 7 day-incubation, with the initial concentration of 300 ppm by high-performance liquid chromatography (HPLC) analysis. To our knowledge, there is rare publication on pyrene degradation by biofilm-forming bacteria. Therefore, the obtained results show that biofilm formed the strain Paracoccus sp. DG25 may considerably increase the degrading efficiency of pyrene and may lead to a new approach to treat polycyclic aromatic hydrocarbons containing in petroleum oil contaminated water in Vietnam. / Trong nghiên cứu này, từ các mẫu đất và nước nhiễm dầu lấy tại kho xăng Đức Giang, Hà Nội, chúng tôi đã phân lập được chủng vi khuẩn có khả năng tạo màng sinh học tốt. Chủng vi khuẩn này đã được phân loại và định tên là Paracoccus sp. DG25 với số đăng ký trên ngân hàng Gen là KJ608354. Chúng tôi cũng đã nghiên cứu một số điều kiện hóa lý ảnh hưởng tới khả năng hình thành màng sinh học như pH, nhiệt độ, nguồn Carbon và nguồn Nitơ. Kết quả cho thấy, chủng DG25 có khả năng tạo màng tốt nhất ở các điều kiện pH 7, 37 oC, nguồn Carbon là maltose và nguồn Nitơ là KNO3. Sử dụng các điều kiện tối ưu này để tạo màng và đánh giá khả năng phân hủy pyrene của màng tạo thành. Bằng phương pháp sắc ký lỏng cao áp, chúng tôi đã đánh giá được hàm lượng pyrene bị phân hủy sau 7 ngày nuôi tĩnh bởi màng sinh học của chủng DG25 lên tới 76,07 % với nồng độ ban đầu là 300 ppm. Cho tới nay, chưa có nhiều công bố về hiệu quả phân hủy pyrene của các chủng vi khuẩn tạo màng sinh học. Do vậy, kết quả đạt được này mở ra khả năng sử dụng màng tạo thành bởi chủng DG25 để nâng cao hiệu quả phân hủy pyren và có thể mở ra phương pháp mới nhằm xử lý các hợp chất hydrocarbon thơm có trong nước ô nhiễm dầu ở Việt Nam.

biologischer Abbau

Biofilm

Paracoccus sp.

Pyrene

biodegradation

biofilm

Paracoccus sp.

pyrene

ddc:363.7

rvk:AR 14000

Characterization of toxicological effects of a novel in vivo benzo[a]pyrene metabolite in colonic cells /

Nordling, Mirjam,

January 2004

Diss. (sammanfattning) Stockholm : Karol. inst., 2004. / Härtill 4 uppsatser.

[en] QUALITATIVE STUDIES FOR DETERMINATION OF PYRENE METABOLITES USING GC/MS / [pt] ESTUDOS QUALITATIVOS PARA DETERMINAÇÃO DE METABÓLITOS DE PIRENO EMPREGANDO CG/EM

PATRICIA RIZEL

23 December 2003

[pt] Os Hidrocarbonetos Policíclicos Aromáticos (HPAs) são contaminantes carcinogênicos e mutagênicos, freqüentemente encontrados no ambiente. Muitos organismos são capazes de metabolizá-los rapidamente, tornando de fundamental importância o desenvolvimento de técnicas analíticas para a determinação de seus metabólitos. A determinação do 1- hidroxipireno é considerada com uma das primeiras etapas para a avaliação do risco ambiental por exposição dos HPAs. O pireno é um dos compostos predominantes desta classe de xenobióticos e o 1-hidroxipireno é o seu principal metabólito. Neste estudo é apresentado uma método para análise qualitativa do 1-hidroxipireno. Testes foram realizados afim de viabilizar a aplicação de uma metodologia para análises de rotina em amostras biológicas. O método escolhido envolve uma etapa de hidrólise ácida com subsequente extração líquido-líquido para obtenção do 1- hidroxipireno. A cromatografia de permeação em gel (CPG) foi empregada como um método de separação de lipídios, seguida de uma etapa de cromatografia líquida de coluna aberta. Uma vez que o 1-hidroxipireno é um composto de baixa volatilidade, foi incluída uma etapa de derivação com BSTFA e seguida de análise por CG/EM. / [en] Polycyclic Aromatic Hydrocarbons are ubiquitous pollutants that usually present carinogenic and mutagenic effects. Several organisms are able to metabolize them quickly, and therefore becoming very important the development of analytical techniques for their metabolites determination. The chemical analyses of 1-hydroxipyrene is one of the first steps for evaluation of environmental assessment by PAH exposure. Pyrene is one of the principal compounds of this xenobiotic class and 1-hydroxipyrene is yours major metabolite. This study presents a method for qualitative analysis of 1-hydroxipirene. Tests were performed due to allow the use of a methodology for routine analysis in biological samples. The chosen method included acid hydrolysis followed of liquid-liquid extraction to obtain 1- hydroxipyrene. Gel permeation chromatography (GPC) was applied as a lipid separation method, and then liquid chromatography of opened column. As long as the 1- hydroxipyrene is a low volatile compound, it was included one step of derivatization with BSTFA followed by gas chromatography/mass spectrometer (GC/MS) analysis.

[pt] UCIDES CORDATUS

[en] UCIDES CORDATUS

[pt] METABOLITOS DE PIRENO

[en] PYRENE METABOLITES

The Synthesis and Characterisation of Polyhedral Oligomeric Silsesquioxane Bound Chromophores

Clarke, David John, d.clarke@irl.cri.nz

January 2008

This research involved the synthesis and characterisation of a range of optically active polyhedral oligomeric silsesquioxane (POSS) compounds. POSS precursor compounds containing functional groups required for subsequent attachment of the desired functional groups have been synthesised. Examples of such precursor compounds include mono-functionalised POSS compounds with periphery aldehyde, azide, amino and pyridyl functional groups. A variety of POSS compounds, functionalised with a range of optical functionalities, including optical limiters such as fulleropyrrolidine and iminofullerene, and dyes and pigments, including naphthalene, biphenyl, perylene, pyrene and porphyrin have been synthesised. The reaction of mono-functionalised POSS aldehydes with fullerene (C60) in the presence of N-methylglycine yielded the desired POSS fulleropyrrolidines, whilst reaction of mono-functionalised POSS azide with C60 yielded POSS iminofullerenes. All POSS fullerene compounds were characterised by power limiting measurements, exhibiting comparable power limiting to that of parent C60. The microwave condensation of mono-amino POSS with a range of mono- and bis-anhydrides yielded the POSS imide compounds, which were characterised by UV-Vis and fluorescence spectrophotometry. The perylene POSS imide derivative was further characterised by single crystal x-ray crystallography. The naphtha and biphenyl POSS imides exhibited extremely weak fluorescence, whilst the perylene ii POSS imide displayed particularly strong fluorescence, with a quantum yield approaching unity. The incorporation of a pyridyl group on the periphery of a mono-functionalised POSS cage allowed for the synthesis of the first porphyrin functionalised POSS compound. Mono-porphyrin POSS exhibited comparable absorption properties to other pyridyl ligated ruthenium porphyrins. Mono-functionalised pyrene POSS compounds were prepared through the reaction of 1-pyrene acid chloride with mono(3-aminopropyl)POSS. This synthetic pathway offered a convenient route to mono-functionalised pyrene POSS, in preference to the multi-substitution associated with Heck coupling. Mono-pyrene POSS was determined to be strongly fluorescent, exhibiting a high quantum yield of fluorescence

silsesquioxane

POSS

fullerene

fulleropyrrolidine

iminofullerene

pyrene

perylene

porphyrin

Mechanisms of environmental tobacco smoke and benzo[a]pyrene induced cardiovascular injury and the protective role of resveratrol

Al-Dissi, Ahmad

21 March 2011

Despite extensive research, the mechanisms behind cardiovascular effects of subchronic environmental tobacco smoke (ETS) remain unclear, but may be related to ETS-induced inflammation and oxidative stress. Additionally, the protective role of resveratrol (RES), a natural antioxidant available in red grapes, is controversial. We hypothesized that the polycyclic aromatic hydrocarbon (PAH) component of ETS is responsible for causing adverse cardiovascular effects. We also hypothesized that the administration of RES is protective against the adverse cardiovascular effects of ETS. In order to address these hypotheses, male juvenile pigs (4-weeks old) were exposed to ETS or ambient air for 28 consecutive days (1 hr/day) and effects compared to 7 days of i.v. injection of the PAH, benzo-a-pyrene (BAP; 5 mg/kg daily). In another experiment, pigs were sham-exposed or ETS-exposed, with or without oral RES treatment (5mg/kg daily). In all experiments, endothelial and left ventricular function were assessed by flow mediated dilation (FMD), and echocardiography, respectively, while blood pressure was evaluated by oscillometry. At the termination of each experiment, serum nitrotyrosine, total nitrate/nitrite (NOx) and C-reactive protein (CRP) were measured as well as hepatic and pulmonary ethoxyresorufin-o-deethylase (EROD) activity to indicate cytochrome P450 1A1 (CYP1A1) expression. Finally, the correlation between pulmonary inflammation and adverse cardiovascular effects was investigated by measuring total and differential white blood cell (WBC) count as well as leukocyte elastase activity in bronchoalveolar lavage fluid at the termination of each experiment. ETS exposure, but not BAP treatment, resulted in a significant impairment of FMD (P<0.0001) and increased left ventricular end diastolic volume (P=0.0032). Cotreatment with RES failed to restore the ETS induced impairment of FMD (P>0.05). However, a trend pointing to an increase in ejection fraction (EF) was noted (P=0.072). ETS, BAP and RES treatments failed to have any effect on blood pressure (P>0.05). BAP injection caused a significant increase in serum nitrotyrosine (P=0.0146) and CRP (P=0.012), but not serum NOx levels (P>0.05). In contrast, ETS exposure resulted in a significant increase in CRP serum levels (P=0.0092), a trend pointing to increased serum nitrotyrosine (P=0.105), and no change in serum NOx levels (P>0.05). The increased nitrotyrosine and CRP with ETS exposure was not reversed by RES administration (P>0.05). ETS exposure increased EROD activity in the lung (P=0.0093), but not the liver (P=0.12). In contrast, BAP treatment had the opposite effect (lung EROD: P=0.621, liver EROD: P=0.01), while RES administration had no effect (P>0.05). ETS exposure (P=0.0139), but not BAP treatment (P=0.723), resulted in increased WBC count in BAL fluid which was not affected by RES administration (P>0.05). These results show that ETS exposure causes lung inflammation, systemic inflammation, oxidative stress-mediated inactivation of nitric oxide and impaired endothelial function. In contrast, BAP failed to alter endothelial function, downstream of the lung, despite systemic inflammation and increased oxidative stress. Furthermore, RES failed to restore endothelial function, or decrease systemic inflammation and oxidative stress. Taken together, these results suggest either that pulmonary inflammatory responses or pulmonary increases in CYP1A1 activity may be more important links to endothelial dysfunction than systemic inflammation and nitric oxide bioactivity. The beneficial effects of RES by itself are manifested only at the cardiac level by improving the ejection fraction, but the work in this thesis failed to detect any ability of RES to ameliorate ETS cardiovascular effects.

oxidative stress

cardiovascular

environmental tobacco smoke

benzo[a]pyrene

inflammation

lung

Characterization of the Self-Assembly of Pyrene-Labelled Macromolecules in Water

Siu, Howard Chun-Kui

January 2010

The self-assembly of several pyrene-labelled amphiphilic macromolecules in water was characterized by fluorescence. Information on their self-assembly was obtained by monitoring the level of pyrene aggregation in solution. A measure of the level of association was obtained by determining the fraction of aggregated pyrene of the labelled macromolecules from the global analysis of their monomer and excimer fluorescence decays. Global analysis limits the degrees of freedom of the analysis thus reducing the error on the parameters retrieved from the analysis. Extensive developments in the global analysis of the pyrene monomer and excimer decays enabled the first characterization of the molar absorbance coefficient of the pyrene aggregates formed by aqueous solutions of pyrene-labelled poly(N,N-dimethylacrylamide) (PyPDMA) and poly(ethylene oxide) (PyPEO). The molar absorbance coefficients of the pyrene aggregates determined for PyPDMA and PyPEO were both found to be broader and red-shifted compared to that of unaggregated pyrene. These results agree with observations found in the scientific literature made by using absorption and excitation fluorescence measurements. Attempts to determine the molar absorbance coefficient of pyrene-labelled hydrophobically-modified alkali-swellable emulsion (PyHASE) polymers were unsuccessful. The inability to characterize the pyrene aggregates of PyHASE was attributed to the greater complexity of the PyHASE polymer compared to PyPDMA and PyPEO. For these simpler pyrene-labelled polymers, a protocol has been established which uses the global analysis of the pyrene monomer and excimer decays to determine quantitatively the level of association of pyrene-labelled polymers as well as the molar absorbance coefficient of their aggregates. Changes in the level of aggregation of pyrene-labelled lipids (PLLs) having head groups bearing an alcohol (PSOH) or imido diacetic acid (PSIDA) embedded in 1-palmitoyl-2-oleyl-3-sn-phosphatidylcholines (POPC) or distearylphosphatidylcholine (DSPC) liposomes were probed by fluorescence. Distribution of the PLLs in the fluid POPC membrane was found to be homogeneous while the PLLs phase-separated into amorphous channels created in the DSPC membranes. Multivalent cations Cu2+ and La3+ were found to bind to PSIDA, hindering diffusional encounters between unaggregated PSIDA but leaving the PLL aggregates intact. Using the fluorescence quenching ability of Cu2+, the viscosity of the amorphous channels of the DSPC membrane was determined to be about six times greater than that of the more fluid POPC membrane. Simultaneous rheological and fluorescence measurements were achieved by interfacing a rheometer with time-resolved and steady-state fluorometers using fiber-optic cables. This joint set up enabled the simultaneous rheological and fluorescence measurements of PyHASE solutions having concentrations ranging from 0.5 w/w% to 5 w/w%. The level of association of the PyHASE solutions was tracked using fluorescence at shear rates of 0, 0.1 and 100 s–1. Despite the presence of shear thinning leading to viscosity drops of up to four orders of magnitude, no change in the fluorescence and hence the level of association was observed. The lack of change in level of association implied that the mechanism of shear thinning is due to a switching from inter- to intramolecular association rather than a drop in the level of association. This information will prove useful for future models attempting to predict the rheological behaviour of sheared associative polymers.

polymer

pyrene

self-assembly

fluorescence

rheology

lipids

Chemistry

Mechanisms of environmental tobacco smoke and benzo[a]pyrene induced cardiovascular injury and the protective role of resveratrol

Al-Dissi, Ahmad

21 March 2011

Despite extensive research, the mechanisms behind cardiovascular effects of subchronic environmental tobacco smoke (ETS) remain unclear, but may be related to ETS-induced inflammation and oxidative stress. Additionally, the protective role of resveratrol (RES), a natural antioxidant available in red grapes, is controversial. We hypothesized that the polycyclic aromatic hydrocarbon (PAH) component of ETS is responsible for causing adverse cardiovascular effects. We also hypothesized that the administration of RES is protective against the adverse cardiovascular effects of ETS. In order to address these hypotheses, male juvenile pigs (4-weeks old) were exposed to ETS or ambient air for 28 consecutive days (1 hr/day) and effects compared to 7 days of i.v. injection of the PAH, benzo-a-pyrene (BAP; 5 mg/kg daily). In another experiment, pigs were sham-exposed or ETS-exposed, with or without oral RES treatment (5mg/kg daily). In all experiments, endothelial and left ventricular function were assessed by flow mediated dilation (FMD), and echocardiography, respectively, while blood pressure was evaluated by oscillometry. At the termination of each experiment, serum nitrotyrosine, total nitrate/nitrite (NOx) and C-reactive protein (CRP) were measured as well as hepatic and pulmonary ethoxyresorufin-o-deethylase (EROD) activity to indicate cytochrome P450 1A1 (CYP1A1) expression. Finally, the correlation between pulmonary inflammation and adverse cardiovascular effects was investigated by measuring total and differential white blood cell (WBC) count as well as leukocyte elastase activity in bronchoalveolar lavage fluid at the termination of each experiment. ETS exposure, but not BAP treatment, resulted in a significant impairment of FMD (P<0.0001) and increased left ventricular end diastolic volume (P=0.0032). Cotreatment with RES failed to restore the ETS induced impairment of FMD (P>0.05). However, a trend pointing to an increase in ejection fraction (EF) was noted (P=0.072). ETS, BAP and RES treatments failed to have any effect on blood pressure (P>0.05). BAP injection caused a significant increase in serum nitrotyrosine (P=0.0146) and CRP (P=0.012), but not serum NOx levels (P>0.05). In contrast, ETS exposure resulted in a significant increase in CRP serum levels (P=0.0092), a trend pointing to increased serum nitrotyrosine (P=0.105), and no change in serum NOx levels (P>0.05). The increased nitrotyrosine and CRP with ETS exposure was not reversed by RES administration (P>0.05). ETS exposure increased EROD activity in the lung (P=0.0093), but not the liver (P=0.12). In contrast, BAP treatment had the opposite effect (lung EROD: P=0.621, liver EROD: P=0.01), while RES administration had no effect (P>0.05). ETS exposure (P=0.0139), but not BAP treatment (P=0.723), resulted in increased WBC count in BAL fluid which was not affected by RES administration (P>0.05). These results show that ETS exposure causes lung inflammation, systemic inflammation, oxidative stress-mediated inactivation of nitric oxide and impaired endothelial function. In contrast, BAP failed to alter endothelial function, downstream of the lung, despite systemic inflammation and increased oxidative stress. Furthermore, RES failed to restore endothelial function, or decrease systemic inflammation and oxidative stress. Taken together, these results suggest either that pulmonary inflammatory responses or pulmonary increases in CYP1A1 activity may be more important links to endothelial dysfunction than systemic inflammation and nitric oxide bioactivity. The beneficial effects of RES by itself are manifested only at the cardiac level by improving the ejection fraction, but the work in this thesis failed to detect any ability of RES to ameliorate ETS cardiovascular effects.

oxidative stress

cardiovascular

environmental tobacco smoke

benzo[a]pyrene

inflammation

lung

Acute Toxicity and Sub-Lethal Effects of Non-Point Source Pollutants on Invertebrates

Romano, Jocelyn Ann

07 May 2007

Non-point source pollution is not generated from any single source, rather can arise from a mixture of agricultural, residential, and industrial activities. As a result of these activities millions of tons of chemicals enter into aquatic environments annually with the potential to disrupt the fragile ecosystems existing within. Common anthropogenic compounds most frequently seen in estuarine environments include pesticides, antifoulants, polycyclic aromatic hydrocarbons (PAH), and industrial solvents. This dissertation examines the acute toxicity and sub-lethal effects of diuron, CuPT, B(a)P, and styrene in the mud snail, Ilyanassa obsoleta, the American oyster, Crassostrea virginica, the sea urchin, Lytechinus variegatus, and/or the barnacle, Amphibalanus (= Balanus) amphitrite. In addition, the general effects of non-point source pollution within the Rachel Carson Estuarine Research Reserve (RCERR) were examined at six sites in order to gain a better understanding of the current health of this unique habitat. Of the four compounds tested, only the industrial solvent, styrene, resulted in an LC50 (1341 µg L-1, I. obsoleta) that was within the range of currently reported environmental levels. Diuron and CuPT did not elicit mortality at environmentally relevant concentrations, but did significantly reduce fecundity in I. obsoleta and C. virginica and fertilization success and larval development in L. variegatus. The only notable sub-lethal effect elicited by the PAH, benzo(a)pyrene, was a significant decrease in egg capsule production by I. obsoleta following exposure to concentrations as low as 50 µg L-1. Within the RCERR, animals from Sites 4, 5, and 6 were observed to have significant differences with respect to fecundity, condition index, and/or ECOD activity when compared to conspecific organisms from control Site 1. This is most likely a consequence of their proximity to anthropogenic sources. Large variation in mortality (15-98.9%) was observed when families of A. amphitrite from a single population where exposed to CuPT. It is often difficult to extrapolate data from laboratory findings into natural populations. Frequently the organisms used under laboratory conditions are genetically very similar, while field population can vary with anthropogenic exposure. Caution must be taken when developing protocols for risk assessment to ensure that actual environmental conditions are being represented. / Dissertation

diuron

copper pyrithione

styrene

benzo(a)pyrene

lytechinus variegatus

ilyanassa obsoleta