Click here to close
Hello! We notice that you are using Internet Explorer, which is not supported by Xenbase and may cause the site to display incorrectly.
We suggest using a current version of Chrome,
FireFox, or Safari.
???displayArticle.abstract???
To investigate the role of the leader peptide in modulating secretion from living cells, we injected a synthetic peptide into Xenopus oocytes. The peptide consisted of the NH2-terminal leader sequence of mouse immunoglobulin light chain precursor. We found that the leader peptide has two different roles in regulating secretion from the oocytes. First, it competitively inhibits the synthesis of secretory and membrane proteins but not of cytoplasmic proteins. The inhibition occurs both with oocyte proteins and with proteins directed by coinjected myeloma mRNA. The inhibition reaches a maximum 2 hr after injection and decays within 3 hr. It appears to be mediated through the cell membrane, because 125I-labeled leader peptide segregates into the membrane fraction of microinjected oocytes simultaneously with the interference with methionine incorporation. A second role of the microinjected leader peptide is to induce a rapid acceleration in the rate of export of secretory proteins from the oocyte. The maximal enhancement effect is obtained upon injection of 50 ng of leader peptide per oocyte. It is not merely due to the small size, negative charge, or hydrophobicity of the peptide, because enhanced secretion does not occur when glucagon, poly-L-glutamic acid, or Triton X-100 is injected. Furthermore, immunoreaction of the peptide with specific antibodies prior to microinjection prevents the accelerated export. Our observations indicate that in Xenopus oocytes, the leader peptide is involved in both translocation and later step(s) in the secretory pathway.
Aviv,
Purification of biologically active globin messenger RNA by chromatography on oligothymidylic acid-cellulose.
1972, Pubmed
Aviv,
Purification of biologically active globin messenger RNA by chromatography on oligothymidylic acid-cellulose.
1972,
Pubmed
Bedouelle,
Mutations which alter the function of the signal sequence of the maltose binding protein of Escherichia coli.
1980,
Pubmed
Blobel,
Transfer of proteins across membranes. I. Presence of proteolytically processed and unprocessed nascent immunoglobulin light chains on membrane-bound ribosomes of murine myeloma.
1975,
Pubmed
Bolton,
The labelling of proteins to high specific radioactivities by conjugation to a 125I-containing acylating agent.
1973,
Pubmed
Colman,
Export of proteins from oocytes of Xenopus laevis.
1979,
Pubmed
,
Xenbase
Colman,
The influence of topology and glycosylation on the fate of heterologous secretory proteins made in Xenopus oocytes.
1981,
Pubmed
,
Xenbase
Cuatrecasas,
Protein purification by affinity chromatography. Derivatizations of agarose and polyacrylamide beads.
1970,
Pubmed
Farquhar,
The Golgi apparatus (complex)-(1954-1981)-from artifact to center stage.
1981,
Pubmed
Habener,
Cellular processing of pre-proparathyroid hormone involves rapid hydrolysis of the leader sequence.
1979,
Pubmed
Katz,
Membrane assembly in vitro: synthesis, glycosylation, and asymmetric insertion of a transmembrane protein.
1977,
Pubmed
Kreil,
Transfer of proteins across membranes.
1981,
Pubmed
Laemmli,
Cleavage of structural proteins during the assembly of the head of bacteriophage T4.
1970,
Pubmed
Lane,
The Xenopus oocyte as a surrogate secretory system. The specificity of protein export.
1980,
Pubmed
,
Xenbase
Lane,
Rabbit haemoglobin synthesis in frog cells: the translation of reticulocyte 9 s RNA in frog oocytes.
1971,
Pubmed
Lane,
Sequestration and turnover of guinea-pig milk proteins and chicken ovalbumin in Xenopus oocytes.
1979,
Pubmed
,
Xenbase
Li,
Total synthesis of camel beta-melanotropin by the solid-phase method.
1975,
Pubmed
Majzoub,
Synthetic pre-proparathyroid hormone leader sequence inhibits cell-free processing of placental, parathyroid, and pituitary prehormones.
1980,
Pubmed
Meyer,
Secretory protein translocation across membranes-the role of the "docking protein'.
1982,
Pubmed
Meyer,
Characterization of molecules involved in protein translocation using a specific antibody.
1982,
Pubmed
Milstein,
A possible precursor of immunoglobulin light chains.
1972,
Pubmed
Mohun,
The secretion of proteins in vitro from Xenopus oocytes and their accessory cells: a biochemical and morphological study.
1981,
Pubmed
,
Xenbase
Rapoport,
Intracellular compartmentation and secretion of carp proinsulin synthesized in Xenopus oocytes.
1981,
Pubmed
,
Xenbase
Richter,
Differential capacity for translation and lack of competition between mRNAs that segregate to free and membrane-bound polysomes.
1981,
Pubmed
,
Xenbase
Richter,
The mechanism for increased protein synthesis during Xenopus oocyte maturation.
1982,
Pubmed
,
Xenbase
Sabatini,
Mechanisms for the incorporation of proteins in membranes and organelles.
1982,
Pubmed
Soreq,
Biosynthesis and secretion of catalytically active acetylcholinesterase in Xenopus oocytes microinjected with mRNA from rat brain and from Torpedo electric organ.
1982,
Pubmed
,
Xenbase
Szczesna,
mRNA-dependent synthesis of authentic precursor to human placental lactogen: conversion to its mature hormone form in ascites cell-free extracts.
1976,
Pubmed
Talmadge,
Eukaryotic signal sequence transports insulin antigen in Escherichia coli.
1980,
Pubmed
Walter,
Translocation of proteins across the endoplasmic reticulum. II. Signal recognition protein (SRP) mediates the selective binding to microsomal membranes of in-vitro-assembled polysomes synthesizing secretory protein.
1981,
Pubmed
Walter,
Translocation of proteins across the endoplasmic reticulum. I. Signal recognition protein (SRP) binds to in-vitro-assembled polysomes synthesizing secretory protein.
1981,
Pubmed
Zehavi-Willner,
Subcellular compartmentation of albumin and globin made in oocytes under the direction of injected messenger RNA.
1977,
Pubmed
,
Xenbase
