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Literature DB >> 3128787

Poly(A) site choice rather than splice site choice governs the regulated production of IgM heavy-chain RNAs.

G Galli¹, J Guise, P W Tucker, J R Nevins.

Abstract

Alternative processing of the immunoglobulin mu primary transcript results in regulated production of mRNAs encoding the secreted (microseconds) and membrane-bound (micro m) form of IgM heavy chain during B-cell development. To elucidate the basis for this control, we analyzed the expression of altered forms of the mu transcription unit. Deletion of intron sequence between the microseconds and micro m exons, which reduces the distance between the two poly(A) sites as well as the distance between micro m splice sites, enhances production of micro m RNA. Correct expression is restored by insertion of heterologous sequences, demonstrating that spacing is indeed the critical aspect. The altered spacing appears to affect poly(A) site usage rather than splice site usage, since it was the distance between the poly(A) sites rather than the distance between splice sites that was found to be decisive. Finally, removal of either the C mu 4 splice donor or the m1 splice acceptor, thus eliminating normal micro m splicing, does not increase usage of the microseconds poly(A) site. We therefore conclude that the major factor in determining the ratio of microseconds to micro m is a poly(A) site choice rather than a splicing choice.

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Year: 1988 PMID： 3128787 PMCID： PMC280012 DOI： 10.1073/pnas.85.8.2439

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

12 in total

1. Regulated production of mu m and mu s mRNA requires linkage of the poly(A) addition sites and is dependent on the length of the mu s-mu m intron.

Authors: M L Peterson; R P Perry
Journal: Proc Natl Acad Sci U S A Date: 1986-12 Impact factor: 11.205

2. Relative position and strengths of poly(A) sites as well as transcription termination are critical to membrane versus secreted mu-chain expression during B-cell development.

Authors: G Galli; J W Guise; M A McDevitt; P W Tucker; J R Nevins
Journal: Genes Dev Date: 1987-07 Impact factor: 11.361

Review 3. Complex transcriptional units: diversity in gene expression by alternative RNA processing.

Authors: S E Leff; M G Rosenfeld; R M Evans
Journal: Annu Rev Biochem Date: 1986 Impact factor: 23.643

4. Cell-type specificity of immunoglobulin gene expression is regulated by at least three DNA sequence elements.

Authors: R Grosschedl; D Baltimore
Journal: Cell Date: 1985-07 Impact factor: 41.582

Review 5. The pathway of eukaryotic mRNA formation.

Authors: J R Nevins
Journal: Annu Rev Biochem Date: 1983 Impact factor: 23.643

6. Two mRNAs can be produced from a single immunoglobulin mu gene by alternative RNA processing pathways.

Authors: P Early; J Rogers; M Davis; K Calame; M Bond; R Wall; L Hood
Journal: Cell Date: 1980-06 Impact factor: 41.582

7. Two mRNAs with different 3' ends encode membrane-bound and secreted forms of immunoglobulin mu chain.

Authors: J Rogers; P Early; C Carter; K Calame; M Bond; L Hood; R Wall
Journal: Cell Date: 1980-06 Impact factor: 41.582

8. Synthesis of secreted and membrane-bound immunoglobulin mu heavy chains is directed by mRNAs that differ at their 3' ends.

Authors: F W Alt; A L Bothwell; M Knapp; E Siden; E Mather; M Koshland; D Baltimore
Journal: Cell Date: 1980-06 Impact factor: 41.582

3. Non-snRNP U1A levels decrease during mammalian B-cell differentiation and release the IgM secretory poly(A) site from repression.

Authors: Jianglin Ma; Samuel I Gunderson; Catherine Phillips
Journal: RNA Date: 2006-01 Impact factor: 4.942

4. An RNA-binding protein specifically interacts with a functionally important domain of the downstream element of the simian virus 40 late polyadenylation signal.

Authors: Z W Qian; J Wilusz
Journal: Mol Cell Biol Date: 1991-10 Impact factor: 4.272

8. The regulated production of mu m and mu s mRNA is dependent on the relative efficiencies of mu s poly(A) site usage and the c mu 4-to-M1 splice.

Authors: M L Peterson; R P Perry
Journal: Mol Cell Biol Date: 1989-02 Impact factor: 4.272

Review 9. Reflections on the history of pre-mRNA processing and highlights of current knowledge: a unified picture.

Authors: James E Darnell
Journal: RNA Date: 2013-02-25 Impact factor: 4.942

10. Efficiency of utilization of the simian virus 40 late polyadenylation site: effects of upstream sequences.

Authors: S Carswell; J C Alwine
Journal: Mol Cell Biol Date: 1989-10 Impact factor: 4.272

Poly(A) site choice rather than splice site choice governs the regulated production of IgM heavy-chain RNAs.

1. Regulated production of mu m and mu s mRNA requires linkage of the poly(A) addition sites and is dependent on the length of the mu s-mu m intron.

2. Relative position and strengths of poly(A) sites as well as transcription termination are critical to membrane versus secreted mu-chain expression during B-cell development.

Review 3. Complex transcriptional units: diversity in gene expression by alternative RNA processing.

4. Cell-type specificity of immunoglobulin gene expression is regulated by at least three DNA sequence elements.

Review 5. The pathway of eukaryotic mRNA formation.

6. Two mRNAs can be produced from a single immunoglobulin mu gene by alternative RNA processing pathways.

7. Two mRNAs with different 3' ends encode membrane-bound and secreted forms of immunoglobulin mu chain.

8. Synthesis of secreted and membrane-bound immunoglobulin mu heavy chains is directed by mRNAs that differ at their 3' ends.

9. Phylogenetic conservation of immunoglobulin heavy chains: direct comparison of hamster and mouse Cmu genes.

10. Splice commitment dictates neuron-specific alternative RNA processing in calcitonin/CGRP gene expression.

Review 1. Developmental regulation of immunoglobulin mRNA processing and the IgA response: establishing a paradigm.

2. Regulation of nuclear poly(A) addition controls the expression of immunoglobulin M secretory mRNA.

3. Non-snRNP U1A levels decrease during mammalian B-cell differentiation and release the IgM secretory poly(A) site from repression.

4. An RNA-binding protein specifically interacts with a functionally important domain of the downstream element of the simian virus 40 late polyadenylation signal.

5. Repositioning of an alternative exon sequence of mouse IgM pre-mRNA activates splicing of the preceding intron.

6. Analysis of human papillomavirus type 16 late mRNA 3' processing signals in vitro and in vivo.

7. Sequences upstream of AAUAAA influence poly(A) site selection in a complex transcription unit.

8. The regulated production of mu m and mu s mRNA is dependent on the relative efficiencies of mu s poly(A) site usage and the c mu 4-to-M1 splice.

Review 9. Reflections on the history of pre-mRNA processing and highlights of current knowledge: a unified picture.

10. Efficiency of utilization of the simian virus 40 late polyadenylation site: effects of upstream sequences.