1.Conservation of cis-Regulatory Element Controlling Timely Translation in the 3'-UTR of Selected Mammalian Maternal Transcripts.
Hyun Joo LEE ; Yoonki LIM ; Sang Ho CHANG ; Kwansik MIN ; Ching Tack HAN ; Sue Yun HWANG
Genomics & Informatics 2007;5(4):174-178
		                        		
		                        			
		                        			The earliest stages of mammalian embryogenesis are governed by the activity of maternally inherited transcripts and proteins. Cytoplasmic polyadenylation of selected maternal mRNA has been reported to be a major control mechanism of delayed translation during preimplantation embryogenesis in mice. The presence of cis-elements required for cytoplasmic polyadenylation (e.g., CPE) can serve as a useful tag in the screening of maternal genes partaking in key functions in the transcriptionally dormant egg and early embryo. However, due to its relative simplicity, UA-rich sequences satisfying the canonical rule of known CPE consensus sequences are often found in the 3'-UTR of maternal transcripts that do not actually undergo cytoplasmic polyadenylation. In this study, we developed a method to confirm the validity of candidate CPE sequences in a given gene by a multiplex comparison of 3'-UTR sequences between mammalian homologs. We found that genes undergoing cytoplasmic polyadenylation tend to create a conserved block around the CPE, while CPE-like sequences in the 3'-UTR of genes lacking cytoplasmic polyadenylation do not exhibit such conservation between species. Through this cross-species comparison, we also identified an alternative CPE in the 3'-UTR of tissue-type plasminogen activator (tPA), which is more likely to serve as a functional element. We suggest that verification of CPEs based on sequence conservation can provide a convenient tool for mass screening of factors governing the earliest processes of mammalian embryogenesis.
		                        		
		                        		
		                        		
		                        			Animals
		                        			;
		                        		
		                        			Consensus Sequence
		                        			;
		                        		
		                        			Cytoplasm
		                        			;
		                        		
		                        			Embryonic Development
		                        			;
		                        		
		                        			Embryonic Structures
		                        			;
		                        		
		                        			Female
		                        			;
		                        		
		                        			Mass Screening
		                        			;
		                        		
		                        			Mice
		                        			;
		                        		
		                        			Ovum
		                        			;
		                        		
		                        			Polyadenylation
		                        			;
		                        		
		                        			Pregnancy
		                        			;
		                        		
		                        			RNA, Messenger, Stored
		                        			;
		                        		
		                        			Tissue Plasminogen Activator
		                        			
		                        		
		                        	
            
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