Pearson M A, Hoyme H E, Seaver L H, Rimsza M E
Department of Pediatrics, University of Arizona College of Medicine, Tucson.
Pediatrics. 1994 Feb;93(2):211-5.
To determine if maternal toluene abuse produces any structural or developmental disabilities in the developing fetus, a cohort of toluene-exposed infants was ascertained and examined.
Eighteen infants with a history of in utero toluene exposure were examined at birth. Nine of these infants were reexamined 3 to 36 months after their initial evaluations. The clinical findings in these patients were compared with those of similarly exposed children from the literature and with patients who had the fetal alcohol syndrome.
Thirty-nine percent of all toluene-exposed infants described in this and other studies were born prematurely, and 9% died during the perinatal period. Fifty-four percent were small for gestational age, and 52% exhibited continued postnatal growth deficiency. A 33% incidence of prenatal microcephaly, a 67% incidence of postnatal microcephaly, and an 80% incidence of developmental delay were observed. Eighty-three percent of the patients had craniofacial features similar to the fetal alcohol syndrome, and 89% of these children had other minor anomalies.
Data from the patients herein described and the available scientific literature suggest that the mechanism of alcohol craniofacial teratogenesis may be nonspecific, with a variety of teratogens, including toluene, giving rise to phenotypic facial abnormalities similar to those of the fetal alcohol syndrome. We propose a common mechanism of craniofacial teratogenesis for toluene and alcohol, namely a deficiency of craniofacial neuroepithelium and mesodermal components due to increased embryonic cell death.
为了确定母亲滥用甲苯是否会在发育中的胎儿身上产生任何结构或发育缺陷,确定并检查了一组接触甲苯的婴儿。
对18名有子宫内接触甲苯史的婴儿在出生时进行了检查。其中9名婴儿在初次评估后3至36个月进行了复查。将这些患者的临床发现与文献中类似接触情况的儿童以及患有胎儿酒精综合征的患者的临床发现进行了比较。
在本研究和其他研究中描述的所有接触甲苯的婴儿中,39%早产,9%在围产期死亡。54%的婴儿小于胎龄,52%在出生后持续生长发育迟缓。观察到产前小头畸形的发生率为33%,产后小头畸形的发生率为67%,发育迟缓的发生率为80%。83%的患者具有与胎儿酒精综合征相似的颅面特征,其中89%的儿童有其他轻微异常。
本文所述患者的数据和现有科学文献表明,酒精性颅面致畸机制可能是非特异性的,多种致畸物,包括甲苯,可导致与胎儿酒精综合征相似的表型面部异常。我们提出甲苯和酒精的颅面致畸共同机制,即由于胚胎细胞死亡增加导致颅面神经上皮和中胚层成分缺乏。