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| 1. |
PHYSIOLOGICAL “CONSTANTS” FOR PBPK MODELS FOR PREGNANCY |
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Journal of Toxicology and Environmental Health,
Volume 52,
Issue 5,
1997,
Page 385-401
JohnF. Young,
WilliamS. Branham,
DanielM. Sheehan,
MichaelE. Baker,
WalterD. Wosilait,
RichardH. Luecke,
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摘要:
Physiologically based pharmacokinetic (PBPK) models for pregnancy are inherently more complex than conventional PBPK models due to the growth of the maternal and embryo/ fetal tissues. Physiological parameters such as compartmental volumes or flow rates are relatively constant at any particular time during gestation when an acute experiment might be conducted, but vary greatly throughout the course of gestation (e.g., contrast relative fetal weight during the first month of gestation with the ninth month). Maternal physiological parameters change during gestation, depending upon the particular system; for example, cardiac output increases by -50% during human gestation; plasma protein concentration decreases during pregnancy; overall metabolism remains fairly constant. Maternal compartmental volumes may change by 10–30% embryo/fetal volume increases over a billionfold from conception to birth. Data describing these physiological changes in the human are available from the literature. Human embryo/fetal growth can be well described using the Compertz equation. By contrast, very little of these same types of data is available for the laboratory animal. In the rodent there is a dearth of information during organogenesis as to embryo weights, and even less organ or tissue weight or volume data during embryonic or fetal periods. Allometric modeling offers a reasonable choice to extrapolate (approximately) from humans to animals; validation, however, is confined to comparisons with limited data during the late embryonic and fetal periods of development (after gestation d 11 in the rat and mouse). Embryonic weight measurements are limited by the small size of the embryo and the current state of technology. However, the application of the laser scanning confocal microscope (LSCM) to optically section intact embryos offers the capability of precise structural measurements and computer-generated three-dimensional reconstruction of early embryos. Application of these PBPK models of pregnancy in laboratory animal models at teratogenically sensitive periods of development provides exposure values at specific target tissues. These exposures provide fundamentally important data to help design and interpret molecular probe investigations into mechanisms of teratogenesis.
ISSN:0098-4108
DOI:10.1080/00984109708984072
出版商:Taylor & Francis Group
年代:1997
数据来源: Taylor
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| 2. |
CARBON MONOXIDE AND WATER VAPOR CONTAMINATION OF COMPRESSED BREATHING AIR FOR FIREFIGHTERS AND DIVERS |
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Journal of Toxicology and Environmental Health,
Volume 52,
Issue 5,
1997,
Page 403-423
C. C. Austin,
D. J. Ecobichon,
G. Dussault,
C. Tirado,
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摘要:
Compressed breathing air, used in self-contained breathing apparatus (SCBA) by firefighters and other categories of workers as well as by recreational and commercial divers, is prepared with the aid of high-pressure compressors operating in the range of 5000 psig. There have been reports of unexplained deaths of SCUBA divers and anecdotal accounts of decreased time to exhaustion in firefighters using SCBAs. Compressed breathing air has been found to contain elevated levels of carbon monoxide (CO) and water vapor that are consistent with carboxyhemoglobin (COHb) poisoning and freezing of the user's regulator on the breathing apparatus. The Coburn-Forster-Kane equation (CFK equation) was used to estimate COHb levels at rest and at maximum exercise when exposed to different levels of CO in contaminated breathing air. The results demonstrated that, at maximum exercise, the COHb ranged from 6.0 to 17% with the use of 1 to 4 SCBA cylinders contaminated by 250 ppm CO. Standard operating procedures have been developed at the Montreal Fire Department to minimize the risk of compressed breathing air contamination. Results of the quality analysis/quality control program indicate that implementation of these procedures has improved the quality of the compressed breathing air. Recommendations are made for improvement of the air testing procedures mandated by the Canadian CAN3 180.1-M85 Standard on Compressed Breathing Air and Systems.
ISSN:0098-4108
DOI:10.1080/00984109708984073
出版商:Taylor & Francis Group
年代:1997
数据来源: Taylor
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| 3. |
FAILURE OF MONOCHLOROACETIC ACID AND TRICHLOROACETIC ACID ADMINISTERED IN THE DRINKING WATER TO PRODUCE LIVER CANCER IN MALE F344/N RATS |
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Journal of Toxicology and Environmental Health,
Volume 52,
Issue 5,
1997,
Page 425-445
AnthonyB. DeAngelo,
F. Bernard Daniel,
BernardM. Most,
GregR. Olson,
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摘要:
The chlorinated acetic acids monochloroacetic acid (MCA) and trichloroacetic acid (TCA) are found as chlorine disinfection by-products in finished drinking-water supplies. TCA has been demonstrated to be a mouse liver carcinogen. A chronic study in which male Fischer 344/N rats were exposed for 104 wk to TCA and MCA in the drinking water is described. Animals, 28 d old, were exposed to 0.05, 0.5, or 2 g/L MCA, or 0.05, 0.5, or 5 g/L TCA. The 2.0 g/L MCA was lowered in stages to 1 g/L when the animals began to exhibit signs of toxicity. A time-weighted mean daily MCA concentration (MDC) of 1.1 g/L was calculated over the 104-wk exposure period. Time-weighted mean daily doses (MDD) based upon measured water consumption were 3.5, 26.1, and 59.9 mg/kg/d for 0.05, 0.5, and 1.1 g/L MCA, respectively; TCA MDD were 3.6, 32.5, and 363.8 mg/kg/d. Nonneoplastic hepatic changes were for the most part spontaneous and age related. No evidence of hepatic neoplasia was found at any of the MCA or TCA doses. The incidence of neoplastic lesions at other sites was not enhanced over that in the control group.
ISSN:0098-4108
DOI:10.1080/00984109708984074
出版商:Taylor & Francis Group
年代:1997
数据来源: Taylor
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| 4. |
ASSESSMENT OF ENVIRONMENTAL HAZARDS OF 1,3,5-TRINITROBENZENE |
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Journal of Toxicology and Environmental Health,
Volume 52,
Issue 5,
1997,
Page 447-460
Gunda Reddy,
TirumuruV. Reddy,
Harlal Choudhury,
F. Bernard Daniel,
GlennJ. Leach,
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摘要:
The remedial investigation/feasibility studies conducted at certain Army installations showed a need to clean up contaminated sites, where high levels of ammunition chemicals such as 2,4,6-trinitrotoluene (TNT), 1,3,5-trinitrobenzene (TNB), 1,3-dinitrobenzene (DNB), and their degradation products/metabolites were detected in surface soil and groundwater. TNB is a photodegradation product of TNT; it is not easily degraded, and persists in the environment. The toxicity data on TNB are scanty. Hence the U.S. Environmental Protection Agency in 1988 (U.S. EPA, 1997) developed a reference dose (RfD) for TNB (0.00005 mg/kg/d for chronic toxicity) based on the toxicity of DNB, which is structurally similar to TNB. Since then we have completed acute, subacute, sub-chronic, chronic, reproductive, and developmental toxicity studies and toxicokinetics studies. We have reviewed the mammalian toxicity data for TNB and have determined the no observed adverse effect levels (NOAEL) and low observed adverse effect levels (LOAEL) for subchronic, chronic, reproductive, and developmental toxicity. Based on the newly determined NOAEL and LOAEL values, we have now developed a new RfD for TNB (0.03 mg/kg/d), based on the chronic toxic effects on hematology and histopatho-logical changes in testes and kidney.
ISSN:0098-4108
DOI:10.1080/00984109708984075
出版商:Taylor & Francis Group
年代:1997
数据来源: Taylor
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| 5. |
EFFECT OF CYPERMETHRIN ON ISOLATED MALE AND FEMALE RAT HEPATOCYTES |
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Journal of Toxicology and Environmental Health,
Volume 52,
Issue 5,
1997,
Page 461-474
OsamaS. El-Tawil,
MohamedS. Abdel-Rahman,
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摘要:
Cypermethrin is a synthetic pyrethroid that belongs to a group of insecticides with low mammalian toxicity but high insecticidal activity. The present study was designed to investigate the toxicity of cypermethrin on freshly isolated hepatocytes from male and female rats. Hepatocytes were harvested by a collagenase perfusion technique and were exposed to different concentrations of cypermethrin (100, 200, 400, or 800 ng/2×106 cells) for up to 2 h. Cell viability and the leakage of aspartate transaminase (AST) and alanine transaminase (ALT) were determined throughout the incubation period. The cell viability of the hepatocytes from male and female rats exposed to 400 ng and 800 ng was significantly reduced after 60 and 30 min of incubation, respectively. With cells from female rats, viability was also reduced upon exposure to 200 ng cypermethrin for 2 h. The decrease in cell viability was dose and time dependent. The leakage of ALT and AST was significantly increased with 400 and 800 ng concentrations at 60 and 30 min, respectively. ALT leakage from female hepatocytes was significantly increased at 60 min of incubation with the 200-ng dose, whereas 2 h of incubation was required for the leakage of ALT from the cells of male rats. The present data indicate that cypermethrin has toxic effects on male and female rat hepatocytes in a dose- and time-dependent manner. The data suggest that female rat hepatocytes may be more sensitive to the toxic effects of cypermethrin than male cells.
ISSN:0098-4108
DOI:10.1080/00984109708984076
出版商:Taylor & Francis Group
年代:1997
数据来源: Taylor
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