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Dive into the research topics where Allan J. Robins is active.

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Featured researches published by Allan J. Robins.


Gene | 1994

SECRETION OF EUKARYOTIC GROWTH HORMONES IN ESCHERICHIA COLI IS INFLUENCED BY THE SEQUENCE OF THE MATURE PROTEINS

Keat-Chye Cheah; Sharon J. Harrison; Robert Michael King; Lesley Crocker; Julian R.E. Wells; Allan J. Robins

We report the construction of secretion plasmids expressing the fusion proteins, OmpA::pGH (pSpGH.01) and OmpA::hGH (phGH.01), and compare the secretion of mature porcine growth hormone (pGH) and human growth hormone (hGH) employing Escherichia coli. E. coli [phGH.01] secreted 10-15 micrograms hGH/ml/A600 cells into the periplasmic space, representing 30% of total periplasmic proteins. E. coli [pSpGH.01], however, secreted 30-fold less mature pGH. On the basis that both pSpGH.01 and phGH.01 are stably maintained in E. coli and in vitro transcription/translation data showed equivalent expression of OmpA::pGH and OmpA::hGH precursors, we attribute the higher secretion of hGH to the translocation-competent OmpA::hGH protein configuration. Two OmpA::GHF (growth hormone fusion) precursors, OmpA::GHF.02 and OmpA::GHF.03, both with hGH helix 3/helix 4 together instead of the pGH equivalent, secreted mature proteins as efficiently as OmpA::hGH. We propose that hGH helices 3 and 4 in these OmpA::GHF precursors play a major role in the folding of the precursor to a translocation-competent state, mimicking the translocation-competent nature of the OmpA::hGH precursor.


Journal of Biological Chemistry | 1987

Characterization of the chicken histone H1 gene complement. Generation of a complete set of vertebrate H1 protein sequences.

L S Coles; Allan J. Robins; L K Madley; Julian R.E. Wells


Archive | 2008

STEM CELL AGGREGATE SUSPENSION COMPOSITIONS AND METHODS OF DIFFERENTIATION THEREOF

Chad Green; Xiaojie Yu; Anne Bang; Eugene P. Brandon; Olivia Kelly; Alan D. Agulnick; Emmanuel E. Baetge; Kevin A. D'Amour; Thomas C. Schulz; Allan J. Robins


Archive | 1995

Mice homozygous for an inactivated α 1,3-galactosyl transferase gene

Anthony J. F. d'Apice; Martin J. Pearse; Allan J. Robins; Robert J. Crawford; Peter D. Rathjen


Archive | 2007

Compositions and methods useful for culturing differentiable cells

Allan J. Robins; Thomas C. Schulz


Journal of Biological Chemistry | 1995

A Growth Hormone Agonist Produced by Targeted Mutagenesis at Binding Site 1. EVIDENCE THAT SITE 1 REGULATES BIOACTIVITY

Scott W. Rowlinson; Ross Barnard; Stan Bastiras; Allan J. Robins; Ross I. Brinkworth; Michael J. Waters


Archive | 2004

Compositions and methods for the control, differentiaton and/or manipulation of pluripotent cells through a gamma-secretase signaling pathway

Brian G. Condie; Allan J. Robins; Scott Noggle


Archive | 2006

Embryonic stem cell culture compositions and methods of use thereof

Allan J. Robins; Thomas C. Schulz; Stephen Dalton; E. Edward Baetge; Melissa K. Carpenter


Cloning and Stem Cells | 2004

An Efficient Method for Producing (1,3)-Galactosyltransferase Gene Knockout Pigs

Sharon J. Harrison; Andrew C. Boquest; C. G. Grupen; Renate Faast; Angelo Guildolin; Chris Giannakis; Lesley Crocker; Stephen M. McIlfatrick; Rodney J. Ashman; James Wengle; Ian Lyons; Paul Tolstoshev; Peter J. Cowan; Allan J. Robins; Philip J. O'Connell; Anthony J. F. d'Apice; Mark B. Nottle


Archive | 1997

Pigs and pig cells having an inactivated α 1,3-galactosyl transferase gene

Anthony J. F. d'Apice; Martin J. Pearse; Allan J. Robins; Robert J. Crawford

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Stan Bastiras

University of Queensland

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Martin J. Pearse

St. Vincent's Health System

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