Testicular Toxicity of Candidate Fuel Additive 1,6-Dimethoxyhexane: Comparison with Several Similar Aliphatic Ethers

doi:10.1093/toxsci/kfj002

ToxSci Advance Access originally published online on October 12, 2005
Toxicological Sciences 2006 89(1):304-313; doi:10.1093/toxsci/kfj002

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Testicular Toxicity of Candidate Fuel Additive 1,6-Dimethoxyhexane: Comparison with Several Similar Aliphatic Ethers

Michael G. Wade¹, Raymond Poon, Nanqin Li, Alice Lee, Avril McMahon and Ih Chu

Systemic Toxicology and Pharmacokinetics Section, Environmental and Occupational Toxicology Division, Environmental Health Science Bureau, Health Canada, Ottawa, Ontario, K1A 0L2, Canada

Received August 18, 2005; accepted September 20, 2005

Previous studies of the toxicity of candidate fuel additivesidentified severe testicular toxicity in animals exposed to1,6-dimethoxyhexane (DMH). A series of studies were conductedto characterize the effects of DMH on spermatogenesis and tocompare the effects of DMH with responses to structural similaraliphatic ethers. In the first study, sexually mature male ratswere administered a single dose (600 mg/kg) of DMH, and subsetsof animals were sampled at intervals post exposure (PE). Bothtestis and thymus weight declined steadily after DMH exposure,both being significantly lower than control by 7 days PE. Treatmentwith DMH led, at 24 to 48 h PE, to an increase in dying primaryspermatocytes in seminiferous tubule stages I–IV and stagesXII–XIV, but not intervening stages. The affected cohortof germ cells was seen progressing through the developmentalsequence of spermatogenesis as numbers of dying cells returnedto control levels by 7 days PE, coincident with a significantdecline in the proportion of round spermatids among germ cellsas determined by flow cytometry. Resolution of round spermatidsto control levels by day 21 PE coincided with a reduction incondensed spermatids (homogenization-resistant spermatid nuclei)and was followed at 28 days PE by a significant reduction incauda epididymal sperm counts. Further studies of repeated exposuresto DMH (200 mg · kg^–1 · day^–1, 5 daysper week for 4 weeks) confirmed the significant testis toxicityof this material. In contrast, similar treatment with any ofa variety of structurally similar aliphatic ethers had littleor no impact on testis function. Methoxyacetic acid, previouslyshown to cause rapid death of some meiotic germ cell stages,was found at high concentrations in the urine of DMH-treatedrats but not in rats treated with other ethers, suggesting thatDMH exerts its testis toxicity via metabolism to this substance.These results demonstrate that DMH selectively deletes germcells from the testis At the very early or very late pachytene,diplotene, or M-phase spermatocyte stages, possibly throughconversion to MAA.

Key Words: fuel additives; testis toxicity; spermatogenesis; methoxyacetic acid; pachytene spermatocytes.

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