Daston G P, Rehnberg B F, Carver B, Rogers E H, Kavlock R J
Developmental Biology Division, U.S. Environmental Protection Agency, Research Triangle Park, North Carolina 27711.
Fundam Appl Toxicol. 1988 Oct;11(3):381-400. doi: 10.1016/0272-0590(88)90104-2.
Substances known or suspected to cause subtle or transient anatomical alterations in renal development were administered prenatally or neonatally to rats in order to determine whether they are capable of altering renal functional development. Colchicine alters mitotic activity and cytoskeletal structure and is teratogenic in many species. Since the kidney of the newborn rat undergoes extensive cellular proliferation and nephron differentiation, it is possible that neonatal administration of colchicine may affect nephron development. Dinoseb and methyl salicylate have previously been reported to produce a high incidence of dilated renal pelvis in the term rat fetus. Colchicine was injected sc, at 75 micrograms/kg, to Postnatal Day (PD) 1 Sprague-Dawley rats. Dinoseb was administered ip to pregnant Sprague-Dawley rats on Gestation Days 10-12 at doses of 8 or 10.5 mg/kg/day, and methyl salicylate was administered ip at doses of 200, 250, or 300 mg/kg/day on Gestation Days 11-12. Renal function was examined in pups from immediately after birth through weaning. Maximal urine concentrating ability was measured after DDAVP (desmopressin acetate, a vasopressin analog) injection in suckling rats, and after 24 hr of water deprivation in weanlings. Proximal tubule transport was measured in renal cortical slices. Basal urinary parameters, including urine flow, osmolality, pH, and chloride content, were measured. Colchicine treatment had no effect on body weight or kidney weight. There was a significant decrease in maximal urine osmolality in PD 30 rats measured after 24 hr of water deprivation. The urine concentrating deficit detected in functionally mature PD 30 rats suggests that colchicine treatment during renal histogenesis causes a latent deficit in medullary function in the absence of any gross morphological effects. The 10.5 mg/kg/day dose of dinoseb caused a weight reduction in neonates which persisted after weaning. Urine volume after DDAVP challenge was increased over controls in both dose groups on PD 6, but maximal urine concentration was unaffected. On PD 14, maximal urine concentration after DDAVP injection was decreased in the 10.5 mg/kg/day group. By PD 30, urine concentrating ability was comparable to controls. Renal cortical slices from the 10.5 mg/kg/day dose group had an enhanced ability to accumulate organic anions on PD 3 and 31, but opposite effects were observed in the low-dose group. No other renal functional parameters were altered. Urine osmolality after DDAVP challenge was decreased over controls in the 250 mg/kg/day methyl salicylate group on PD 6, and urine volume was increased in this group after DDAVP injection on PD 14.(ABSTRACT TRUNCATED AT 400 WORDS)
已知或疑似会在肾脏发育过程中引起细微或短暂解剖学改变的物质,在产前或新生期给予大鼠,以确定它们是否能够改变肾脏功能发育。秋水仙碱会改变有丝分裂活性和细胞骨架结构,并且在许多物种中具有致畸性。由于新生大鼠的肾脏会经历广泛的细胞增殖和肾单位分化,因此新生期给予秋水仙碱可能会影响肾单位发育。地乐酚和水杨酸甲酯此前已被报道在足月大鼠胎儿中会导致肾盂扩张的高发生率。对出生后第1天(PD1)的斯普拉格-道利大鼠皮下注射75微克/千克秋水仙碱。在妊娠第10 - 12天,以8或10.5毫克/千克/天的剂量对妊娠的斯普拉格-道利大鼠腹腔注射地乐酚,在妊娠第11 - 12天,以200、250或300毫克/千克/天的剂量腹腔注射水杨酸甲酯。对出生后直至断奶的幼崽进行肾功能检查。在哺乳期大鼠注射醋酸去氨加压素(一种血管加压素类似物)后,以及在断奶幼崽禁水24小时后,测量最大尿浓缩能力。在肾皮质切片中测量近端小管转运。测量基础尿液参数,包括尿流量、渗透压、pH值和氯含量。秋水仙碱处理对体重或肾脏重量没有影响。在禁水24小时后测量的PD30大鼠中,最大尿渗透压显著降低。在功能成熟的PD30大鼠中检测到的尿浓缩缺陷表明,在肾脏组织发生过程中进行秋水仙碱处理会在没有任何明显形态学影响的情况下导致髓质功能的潜在缺陷。10.5毫克/千克/天剂量的地乐酚导致新生大鼠体重减轻,断奶后仍持续存在。在PD6时,两个剂量组在注射醋酸去氨加压素后的尿量均高于对照组,但最大尿浓缩能力未受影响。在PD14时,10.5毫克/千克/天组在注射醋酸去氨加压素后的最大尿浓缩能力降低。到PD30时,尿浓缩能力与对照组相当。在PD3和31时,10.5毫克/千克/天剂量组的肾皮质切片积累有机阴离子的能力增强,但在低剂量组观察到相反的效果。没有其他肾功能参数发生改变。在PD6时,250毫克/千克/天水杨酸甲酯组在注射醋酸去氨加压素后的尿渗透压低于对照组,在PD14时,该组在注射醋酸去氨加压素后的尿量增加。(摘要截断于400字)
