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借助肢体培养和图像分析对羟基脲与5-溴脱氧尿苷的致畸相互作用进行了研究。

The teratogenic interaction of hydroxyurea and 5-bromodeoxyuridine examined with the aid of limb culture and image analysis.

作者信息

Kwasigroch T E, Skalko R G

出版信息

Fundam Appl Toxicol. 1985 Dec;5(6 Pt 1):1161-73. doi: 10.1016/0272-0590(85)90153-8.

Abstract

Pregnant mice were treated on gestation Day 11 (E11) with a single dose of either hydroxyurea (HU, 250 mg/kg) or 5-bromo-2'deoxyuridine (BrdU, 500 mg/kg), or with a combination of the two agents. The dams were either allowed to go to term, when the fetuses were examined for cleft palate (CP) and digital anomalies, or killed 24 hr after the treatment. In the latter case, limbs from the embryos of control and treated dams were excised and cultured for 6 days in submerged culture. At the end of the culture period, the limb explants were stained for cartilage. The various cartilaginous components were subsequently analyzed using image analysis methods. CP was observed in 2.4 and 22.9% of the fetuses, respectively, after a single dose of HU or BrdU on E11. Simultaneous HU + BrdU treatment decreased the incidence of BrdU-induced CP to 3.6%, while treatment with BrdU 3 hr after HU resulted in 33.3% CP. In addition, syndactyly and ectrodactyly, not seen after the treatment with either HU or BrdU alone, were observed when the two agents were administered simultaneously, 1 hr apart or with a 3-hr delay. The teratogenic response was enhanced when limbs were cultured for 6 days. Digital anomalies were observed in the limb explants of BrdU-pretreated embryos; such abnormalities were not observed in vivo. Image analysis of cultured limb explants revealed that with HU-3 hr-BrdU pretreatment, the total limb area occupied by the long bones was increased at the cost of the paw area. However, no consistent changes in the shape or form of individual bones were observed. HU and BrdU given together produced a teratogenic response which was significantly different from that observed following the administration of HU or BrdU alone. This is considered to be due to an interference with the incorporation of BrdU in the DNA, since HU is known to block DNA synthesis. When HU was given before BrdU, the effects of BrdU were enhanced, probably due to the reported synchronizing action of HU on dividing cells. We also found that after a similar in utero exposure, the culture conditions themselves enhanced the frequency of teratogenic expression of BrdU.

摘要

在妊娠第11天(E11),给怀孕小鼠单次注射羟基脲(HU,250毫克/千克)或5-溴-2'-脱氧尿苷(BrdU,500毫克/千克),或同时注射这两种药物。让母鼠足月分娩,检查胎儿是否有腭裂(CP)和手指异常,或者在治疗后24小时处死母鼠。在后一种情况下,将对照母鼠和处理过的母鼠胚胎的肢体切除,并在浸没培养中培养6天。培养期结束时,对肢体外植体进行软骨染色。随后使用图像分析方法分析各种软骨成分。在E11单次注射HU或BrdU后,分别在2.4%和22.9%的胎儿中观察到CP。同时给予HU + BrdU治疗可将BrdU诱导的CP发生率降至3.6%,而在HU后3小时给予BrdU则导致33.3%的CP发生率。此外,当同时给予这两种药物、间隔1小时或延迟3小时给药时,观察到单独使用HU或BrdU治疗后未出现的并指和缺指畸形。当肢体培养6天时,致畸反应增强。在BrdU预处理胚胎的肢体外植体中观察到手指异常;在体内未观察到此类异常。对培养的肢体外植体进行图像分析发现,经过HU-3小时-BrdU预处理后,长骨占据的肢体总面积增加,而爪部面积减小。然而,未观察到单个骨骼的形状或形态有一致变化。HU和BrdU联合使用产生的致畸反应与单独给予HU或BrdU后观察到的反应显著不同。这被认为是由于HU干扰了BrdU掺入DNA,因为已知HU会阻断DNA合成。当在BrdU之前给予HU时,BrdU的作用增强,可能是由于HU对分裂细胞具有同步作用。我们还发现,在类似的子宫内暴露后,培养条件本身会增加BrdU致畸表达的频率。

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