Functional Activity of Mouse Sperm Was Not Affected by Low Doses of Aspirin-Like Drugs

Stutz, G.; Martini, Ana Carolina; Ruiz, Rubén Daniel; Cúneo, Marta Fiol de; Muñoz, Liliana; Lacuara, J. L.

doi:10.1080/014850100262281

Cited by 18 publications

(6 citation statements)

References 24 publications

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“…Similar effects on gonad development and reproductive health of F0 adult female rodents have been described after exposure to high doses of APAP or indomethacin (26,27). However, fertility of adult male rats (26) and sperm parameters in mice (25) were not altered by exposure in utero to these drugs.…”

Section: Discussionsupporting

confidence: 58%

“…Moreover, in adult rats, long-term treatment with APAP at high doses impairs sexual competence, sperm count and quality, and fertility (24). Conversely, adult mouse sperm parameters are not affected after in utero exposure to low doses of ASA or IBU (25). Similarly, in vivo administration of APAP or indomethacin to pregnant rats during embryogenesis decreases the number of fetal germ cells and accelerates their embryonic differentiation but does not affect the fertility of adult male rats (26).…”

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confidence: 99%

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Intergenerational effects on mouse sperm quality after in utero exposure to acetaminophen and ibuprofen

et al. 2018

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Nonsteroidal antiinflammatory drugs and analgesic drugs, such as N-acetyl- p-aminophenol (APAP; acetaminophen, paracetamol), are widely used by pregnant women. Accumulating evidence has indicated that these molecules can favor genital malformations in newborn boys and reproductive disorders in adults. However, the consequences on postnatal testis development and adult reproductive health after exposure during early embryogenesis are still unknown. Using the mouse model, we show that in utero exposure to therapeutic doses of the widely used APAP-ibuprofen combination during the sex determination period leads to early differentiation and decreased proliferation of male embryonic germ cells, and early 5-methylcytosine and extracellular matrix protein deposition in 13.5 d postcoitum exposed testes. Consequently, in postnatal testes, Sertoli-cell maturation is delayed, the Leydig-cell compartment is hyperplasic, and the spermatogonia A pool is decreased. This results in a reduced production of testosterone and in epididymal sperm parameter defects. We observed a reduced sperm count (19%) in utero-exposed (F0) adult males and also a reduced sperm motility (40%) in their offspring (F1) when both parents were exposed, which leads to subfertility among the 6 mo old F1 animals. Our study suggests that the use of these drugs during the critical period of sex determination affects the germ-line development and leads to adverse effects that could be passed to the offspring.-Rossitto, M., Marchive, C., Pruvost, A., Sellem, E., Ghettas, A., Badiou, S., Sutra, T., Poulat, F., Philibert, P., Boizet-Bonhoure, B. Intergenerational effects on mouse sperm quality after in utero exposure to acetaminophen and ibuprofen.

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Section: Discussionsupporting

confidence: 58%

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confidence: 99%

Intergenerational effects on mouse sperm quality after in utero exposure to acetaminophen and ibuprofen

et al. 2018

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“…Though, in contrast, only one animal study conducted on rams showed improvement in sperm motility after aspirin supplementation at 75 mg/kg, for 4 days, however, in this study other sperm markers such as count and volume were negatively affected (Tanyildizi & Bozkurt, 2003). Alternatively, there was a blunted effect on sperm motility and viability after administration of aspirin at 14.3 mg kg −1 day −1 , for 35 and 60 days, in adult mouse males (Stutz et al, 2000).…”

Section: Ta B L Econtrasting

confidence: 80%

Aspirin decreases human sperm motility and vitality, chelates seminal calcium, but insignificantly reduces seminal nitric oxide production

Banihani

Shatnawi

2020

Andrologia

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Aspirin (2-acetoxybenzoic acid), or acetylsalicylic acid, is an anti-inflammatory, analgesic and antipyretic medication (Banihani, 2019; Yin, Yamamoto, & Gaynor, 1998). It is one of the nonsteroidal anti-inflammatory drugs (NSAIDs) (Webb et al., 2019). Currently, aspirin is extensively used to increase the thinning effect of the blood or reduce the blood clots as it inhibits the function of platelets (Jia et al., 2019; Shen et al., 2019; Xu et al., 2019). Therefore, as urgent medical practice, to reduce the risk of death, aspirin is highly recommended just after the event of a heart attack (Dalen, 2006; McNeil et al., 2018). However, recurrent use of aspirin has been found to have serious adverse effects such as stomach bleeding and stomach ulcer (Chen et al., 2017; Taha, McCloskey, McSkimming, & McConnachie, 2018). Biochemically, aspirin suppresses the formation of prostaglandins and thromboxanes (Gimenez-Bastida, Boeglin, Boutaud, Malkowski, & Schneider, 2019; Rauzi et al., 2016) since it irreversibly inactivates cyclooxygenase (prostaglandin-endoperoxide synthase), which is an enzyme that catalyses the formation of prostanoids such as prostaglandins (e.g. prostacyclin) and thromboxane from

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“…The present study represents the first GC/MS-MS global analysis of fetal testicular steroidogenesis demonstrating that, in addition to suppression of testosterone, the effect of ibuprofen on the expression of CYP17A1 also negatively impacted androstenedione and to a greater extent 5α-DHT. Further supporting evidence for ibuprofen being an anti-androgenic compound is the observation that low doses of this NSAID (5–6 mg/kg/day for 35 days) inhibited plasma levels of testosterone in adult male mice59. Ibuprofen has also been shown to inhibit the human UDP-glucuronosyltransferases UGT2B15 and UGT2B17, and the latter is very important for glucuronidation and testosterone excretion60.…”

Section: Discussionmentioning

confidence: 96%

Ibuprofen results in alterations of human fetal testis development

Maamar

Lesné

Hennig

et al. 2017

Sci Rep

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Among pregnant women ibuprofen is one of the most frequently used pharmaceutical compounds with up to 28% reporting use. Regardless of this, it remains unknown whether ibuprofen could act as an endocrine disruptor as reported for fellow analgesics paracetamol and aspirin. To investigate this, we exposed human fetal testes (7–17 gestational weeks (GW)) to ibuprofen using ex vivo culture and xenograft systems. Ibuprofen suppressed testosterone and Leydig cell hormone INSL3 during culture of 8–9 GW fetal testes with concomitant reduction in expression of the steroidogenic enzymes CYP11A1, CYP17A1 and HSD17B3, and of INSL3. Testosterone was not suppressed in testes from fetuses younger than 8 GW, older than 10–12 GW, or in second trimester xenografted testes (14–17 GW). Ex vivo, ibuprofen also affected Sertoli cell by suppressing AMH production and mRNA expression of AMH, SOX9, DHH, and COL2A1. While PGE2 production was suppressed by ibuprofen, PGD2 production was not. Germ cell transcripts POU5F1, TFAP2C, LIN28A, ALPP and KIT were also reduced by ibuprofen. We conclude that, at concentrations relevant to human exposure and within a particular narrow ‘early window’ of sensitivity within first trimester, ibuprofen causes direct endocrine disturbances in the human fetal testis and alteration of the germ cell biology.

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Functional Activity of Mouse Sperm Was Not Affected by Low Doses of Aspirin-Like Drugs

Cited by 18 publications

References 24 publications

Intergenerational effects on mouse sperm quality after in utero exposure to acetaminophen and ibuprofen

Intergenerational effects on mouse sperm quality after in utero exposure to acetaminophen and ibuprofen

Aspirin decreases human sperm motility and vitality, chelates seminal calcium, but insignificantly reduces seminal nitric oxide production

Ibuprofen results in alterations of human fetal testis development

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