TY - JOUR
T1 - Effect of inhibition of sterol Δ14-reductase on accumulation of meiosis-activating sterol and meiotic resumption in cumulus-enclosed mouse oocytes in vitro
AU - Leonardsen, Lise
AU - Strømstedt, Maria
AU - Jacobsen, Ditte
AU - Kristensen, Karina S.
AU - Baltsen, Mogens
AU - Andersen, Claus Yding
AU - Byskov, Anne Grete
PY - 2000/1
Y1 - 2000/1
N2 - Two sterols of the cholesterol biosynthetic pathway induce resumption of meiosis in mouse oocytes in vitro. The sterols, termed meiosis-activating sterols (MAS), have been isolated from human follicular fluid (FF-MAS, 4,4-dimethyl-5α-cholest-8,14,24-triene-3β-ol) and from bull testicular tissue (T-MAS, 4,4-dimethyl-5α-cholest-8,24-diene-3β-ol). FF-MAS is the first intermediate in the cholesterol biosynthesis from lanosterol and is converted to T-MAS by sterol Δ14-reductase. An inhibitor of Δ7-reductase and Δ14 reductase, AY9944-A-7, causes cells with a constitutive cholesterol biosynthesis to accumulate FF-MAS and possibly other intermediates between lanosterol and cholesterol. The aim of the present study was to evaluate whether AY9944-A-7 added to cultures of cumulus-oocyte complexes (COC) from mice resulted in accumulation of MAS and meiotic maturation. AY9944-A-7 stimulated dose dependently (5-25 μmol l
-1) COC to resume meiosis when cultured for 22 h in α minimal essential medium (α-MEM) containing 4 mmol hypoxanthine l
-1, a natural inhibitor of meiotic maturation. In contrast, naked oocytes were not induced to resume meiosis by AY9944-A-7. When cumulus cells were separated from their oocytes and co-cultured, AY9944-A-7 did not affect resumption of meiosis, indicating that intact oocyte-cumulus cell connections are important for AY9944-A-7 to exert its effect on meiosis. Cultures of COC with 10 μmol AY9944-A-7 l
-1 in the presence of [
3H]mevalonic acid, a natural precursor for steroid synthesis, resulted in accumulation of labelled FF-MAS, which had an 11-fold greater amount of radioactivity incorporated per COC compared with the control culture without AY9944-A-7. In contrast, incorporation of radioactivity into the cholesterol fraction was reduced 30-fold in extracts from the same oocytes. The present findings demonstrate for the first time that COC can synthesize cholesterol from mevalonate and accumulate FF-MAS in the presence of AY9944-A-7. Furthermore, AY9944-A-7 stimulated meiotic maturation dose dependently, indicating that FF-MAS, and possibly other sterol intermediates of the cholesterol synthesis pathway, play a central role in stimulating mouse oocytes to resume meiosis. The results also indicate that oocytes may not synthesize steroids from mevalonate.
AB - Two sterols of the cholesterol biosynthetic pathway induce resumption of meiosis in mouse oocytes in vitro. The sterols, termed meiosis-activating sterols (MAS), have been isolated from human follicular fluid (FF-MAS, 4,4-dimethyl-5α-cholest-8,14,24-triene-3β-ol) and from bull testicular tissue (T-MAS, 4,4-dimethyl-5α-cholest-8,24-diene-3β-ol). FF-MAS is the first intermediate in the cholesterol biosynthesis from lanosterol and is converted to T-MAS by sterol Δ14-reductase. An inhibitor of Δ7-reductase and Δ14 reductase, AY9944-A-7, causes cells with a constitutive cholesterol biosynthesis to accumulate FF-MAS and possibly other intermediates between lanosterol and cholesterol. The aim of the present study was to evaluate whether AY9944-A-7 added to cultures of cumulus-oocyte complexes (COC) from mice resulted in accumulation of MAS and meiotic maturation. AY9944-A-7 stimulated dose dependently (5-25 μmol l
-1) COC to resume meiosis when cultured for 22 h in α minimal essential medium (α-MEM) containing 4 mmol hypoxanthine l
-1, a natural inhibitor of meiotic maturation. In contrast, naked oocytes were not induced to resume meiosis by AY9944-A-7. When cumulus cells were separated from their oocytes and co-cultured, AY9944-A-7 did not affect resumption of meiosis, indicating that intact oocyte-cumulus cell connections are important for AY9944-A-7 to exert its effect on meiosis. Cultures of COC with 10 μmol AY9944-A-7 l
-1 in the presence of [
3H]mevalonic acid, a natural precursor for steroid synthesis, resulted in accumulation of labelled FF-MAS, which had an 11-fold greater amount of radioactivity incorporated per COC compared with the control culture without AY9944-A-7. In contrast, incorporation of radioactivity into the cholesterol fraction was reduced 30-fold in extracts from the same oocytes. The present findings demonstrate for the first time that COC can synthesize cholesterol from mevalonate and accumulate FF-MAS in the presence of AY9944-A-7. Furthermore, AY9944-A-7 stimulated meiotic maturation dose dependently, indicating that FF-MAS, and possibly other sterol intermediates of the cholesterol synthesis pathway, play a central role in stimulating mouse oocytes to resume meiosis. The results also indicate that oocytes may not synthesize steroids from mevalonate.
KW - disease, health science and nursing
UR - http://www.scopus.com/inward/record.url?scp=0342680059&partnerID=8YFLogxK
U2 - 10.1530/reprod/118.1.171
DO - 10.1530/reprod/118.1.171
M3 - Journal article
SN - 0022-4251
VL - 118
SP - 171
EP - 179
JO - Journal of Reproduction and Fertility
JF - Journal of Reproduction and Fertility
IS - 1
ER -