In view of the importance and beneficial characteristics of enantioenriched tertiary alcohols in pharmaceutical chemistry, efficient and green strategies for their synthesis are highly sought after. Here, we report a simple synthesis of the elusive chiral tertiary alcohols. A cytochrome P450 monooxygenase called P450PL2 was developed to enable chiral tertiary alcohols by the benzylic CH bonds asymmetric hydroxylation of the racemic tertiary carbon substrates. This P450-catalyzed protocol provides various chiral tertiary alcohols with unexpectedly functional group tolerance and excellent enantioselectivities (up to >99 % ee). The method features mild reaction and employs molecular oxygen as an oxidant, avoids the use of pre-oxygen functionalized substrates. Preliminary molecular dynamics simulation studies were carried out to reveal the possible reasons for the exceptional selective hydroxylation of substrate during P450PL2 catalysis.