TY - JOUR
T1 - An autoantibody derived from mice with experimental systemic lupus erythematosus is directed against the essential splicing factor SF53/4-a possible role for large nuclear ribonucleoprotein particles in autoimmune disorders
AU - Ast, Gil
AU - Goldblatt, Drora
AU - Waisman, Ari
AU - Sperling, Ruth
AU - Mozes, Edna
AU - Sperling, Joseph
PY - 1994/8
Y1 - 1994/8
N2 - We have previously shown that nuclear transcripts of several pre-mRNAs can be released from nuclei of mammalian cells in a form of large nuclear ribonucleoprotein (InRNP) particles. These particles, which invariably sediment at the 200S region in sucrose gradient, contain all U small nuclear RNPs required for pre-mRNA splicing and a multitude of heterogeneous nuclear RNP proteins. From a panel of mAbs raised against the inRNP particles, a specific mAb (53/4) identified a nuclear protein of 88 kDa as an essential splicing factor (SF53/4). In a parallel independent study, mAbs were established in mice with experimental systemic lupus erythematosus (SLE), that had been induced by immunization with a murine mAb against a human anti-DNA mAb bearing the common 16/6 idiotype. One of the produced mAbs (2C5/3) recognized an 88 kDa RNP protein. In the present study we have used the following criteria to demonstrate that mAb 2C5/3 and mAb 53/4 recognize the same protein. First, mAb 2C5/3 inhibited splicing by direct addition. Second, the 88 kDa polypeptide that had been immunodepleted from HeLa cells nuclear extract by mAb 2C5/3 was recognized by mAb 53/4 in protein blots. Third, the HeLa nuclear extract depleted by mAb 2C5/3 was devoid of splicing activity and could not assemble into splicing complexes with exogenous pre-mRNA; however, splicing and spliceosome assembly activities were restored to such a defective extract by adding back the 88 kDa protein that had been purified by immunoaffinity binding to immobilized mAb 53/4. These results demonstrate that mAb 2C5/3, which was derived from mice with experimental SLE, is directed against epitope(s) involved in the activity of SF53/4. The fact that SF53/4 is an integral component of the InRNP particles implies the possibility that such particles are involved in eliciting an autoimmune response.
AB - We have previously shown that nuclear transcripts of several pre-mRNAs can be released from nuclei of mammalian cells in a form of large nuclear ribonucleoprotein (InRNP) particles. These particles, which invariably sediment at the 200S region in sucrose gradient, contain all U small nuclear RNPs required for pre-mRNA splicing and a multitude of heterogeneous nuclear RNP proteins. From a panel of mAbs raised against the inRNP particles, a specific mAb (53/4) identified a nuclear protein of 88 kDa as an essential splicing factor (SF53/4). In a parallel independent study, mAbs were established in mice with experimental systemic lupus erythematosus (SLE), that had been induced by immunization with a murine mAb against a human anti-DNA mAb bearing the common 16/6 idiotype. One of the produced mAbs (2C5/3) recognized an 88 kDa RNP protein. In the present study we have used the following criteria to demonstrate that mAb 2C5/3 and mAb 53/4 recognize the same protein. First, mAb 2C5/3 inhibited splicing by direct addition. Second, the 88 kDa polypeptide that had been immunodepleted from HeLa cells nuclear extract by mAb 2C5/3 was recognized by mAb 53/4 in protein blots. Third, the HeLa nuclear extract depleted by mAb 2C5/3 was devoid of splicing activity and could not assemble into splicing complexes with exogenous pre-mRNA; however, splicing and spliceosome assembly activities were restored to such a defective extract by adding back the 88 kDa protein that had been purified by immunoaffinity binding to immobilized mAb 53/4. These results demonstrate that mAb 2C5/3, which was derived from mice with experimental SLE, is directed against epitope(s) involved in the activity of SF53/4. The fact that SF53/4 is an integral component of the InRNP particles implies the possibility that such particles are involved in eliciting an autoimmune response.
KW - Autoimmunity
KW - Monocional antibodies
KW - Pre-mRNA splicing
KW - RNP particles
KW - Spliceosome
UR - http://www.scopus.com/inward/record.url?scp=0028068836&partnerID=8YFLogxK
U2 - 10.1093/intimm/6.8.1097
DO - 10.1093/intimm/6.8.1097
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C2 - 7981139
AN - SCOPUS:0028068836
SN - 0953-8178
VL - 6
SP - 1097
EP - 1105
JO - International Immunology
JF - International Immunology
IS - 8
ER -