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To gain an insight into the relationship between the time in which a daily UV dose is delivered and its carcinogenic effectiveness, the following experiment was performed. Three groups of 24 albino hairless mice (Skh-hr1) were exposed to the same daily dose of UVB radiation (600 J m-2; Philips TL12). The exposure times for the three groups were 1.25, 4 and 12 h per day. A fourth unirradiated group served as a control. All animals exposed to UVB developed multiple skin tumours, whereas the control animals did not develop any observable tumours. Tumour development in the groups exposed for 4 and 12 h was virtually identical. Tumour development was significantly faster in the groups exposed for 4 and 12 h per day than in the group exposed for 1.25 h: the median tumour induction time was reduced by 12%. In terms of the effective dose, this is equivalent to a 25% increase in effectiveness for the 4 and 12 h groups relative to the 1.25 h group. In conclusion, the present experiment shows that prolongation of the exposure duration increases the carcinogenic efficacy of UVB radiation.  相似文献   
2.
Exposure of the skin to UV radiation can lead to a local infiltration of neutrophils. Not much is known on whether the infiltration of neutrophils in the irradiated skin is UV source dependent. In this study we compared different UV sources (solar-simulated radiation [SSR], narrowband [NB]-UVB, broadband [BB]-UVB and UVA1) in their potency to induce neutrophil infiltration in normal human skin after exposure to two times the minimal erythema dose of UV radiation. Biopsies were collected from irradiated buttock skin 6 and 24 h after irradiation and from nonirradiated skin. The presence, distribution and amount of skin-infiltrated neutrophils were determined using immunohistochemical staining. Analysis revealed that SSR was most effective in inducing neutrophil infiltration. NB-UVB gave a neutrophil influx pattern similar to that seen with SSR but in smaller numbers. BB-UVB and UVA1 were far less potent in inducing neutrophil infiltration compared with SSR or NB-UVB. Our findings indicate that neutrophil infiltration in the UV-irradiated skin is UV source dependent. When the spectra emitted by the different UV sources were compared UVB seemed to be more effective than UVA in inducing neutrophil infiltration. Furthermore, our results suggest that longer wavelengths within the UVB range are mostly responsible for the infiltration of neutrophils in the UV-irradiated skin.  相似文献   
3.
We have earlier reported on determining UV-induced DNA damage in murine epidermal cell suspensions by flow cytometric analysis of the fluorescence from a fluorescein isothiocyanate-labeled antibody (H3) directed against thymine dimers (T>2-M-phase cells can further be distinguished from cell doublets by pulse-shape discrimination. Thus, T>(i.e. G0-G1, S or G2-M phases) can be determined after in vivo exposure of human skin to environmentally relevant UVB (280–315nm) doses. The method was applied to measure the decrease of T>0-G1 phase) and replicating cells (S phase or G2-M phase) from seven volunteers exposed to twice their minimal erythema dose. The reduction in the average T>0-G1 cells and 70% (ranging between 37% and 100%) for the S + G2-M cells. The difference was statistically highly significant. Determination of individual DNA repair capacities with this method can become a convenient diagnostic tool for patients with DNA repair disorders, or it may even be used to identify individuals with low repair proficiencies and increased risk of developing skin cancers.  相似文献   
4.
Groups of hairless mice were irradiated daily with Philips TL01 UVB sources. This type of lamp has become available recently and was developed for UVB phototherapy of psoriasis. The TL01 emits radiation in a narrow band around 311-312 nm. Tumours developed on all animals. The dose-response relationship had practically the same shape as that found in a similar experiment with Westinghouse FS40 sunlamps; the tumour induction time appeared to be proportional to the daily dose to a power of -0.58. An additional experiment was performed with a TL01 from which the shorter wavelengths were filtered away. This reduced the carcinogenic effectiveness by a factor of 2.3. The potential of the filtered lamp for phototherapy of psoriasis is discussed.  相似文献   
5.
Abstract— The extent to which transmission of human Caucasian epidermis and stratum corneum influences the Minimal Erythema Dose (MED) was examined for UV-B and UV-C.
Transmission correlated well with variations in MED for UV-B and UV-C that exist between individuals, as measured on the skin of the lower back and anterior upper leg.
Regional differences of the MED that occur within the same individual between different parts of the body, were related less well to differences in transmission. For UV-B, the difference in transmission of stratum corneum and epidermis between upper leg and lower back was on the average too small to completely account for the difference in MED UV-B. Other parameters, therefore, have to be involved in determining such regional variations in MED UV-B. For UV-C, on average, the difference in transmission of stratum corneum was smaller and of epidermis larger than the difference in MED UV-C between upper leg and lower back, though the deviations were not significant.
A series of UV-B irradiations of the lower back resulted in an increase in MED UV-B and MED UV-C, which was paralleled by a decrease in transmission of stratum corneum and epidermis. The average decrease in UV-B transmission of stratum corneum was too small and that of epidermis somewhat too large to account for the average increase in MED UV-B. The average decrease in UV-C transmission of stratum corneum was about as large as the average increase in MED UV-C. Consequences of these observations for the location of the primary reactions leading to erythema are discussed.
The relationship between log MED UV-C and log MED UV-B was confirmed to be approximately linear.  相似文献   
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