Joacim Elmén
Karolinska Institutet
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Publication
Featured researches published by Joacim Elmén.
Biochemical and Biophysical Research Communications | 2003
Yunhe Xu; Hong Yan Zhang; Dorit Thormeyer; Ola Larsson; Quan Du; Joacim Elmén; Claes Wahlestedt; Zicai Liang
Antisense DNA target sites can be selected by the accessibility of the mRNA target. It remains unknown whether a mRNA site that is accessible to an antisense DNA is also a good candidate target site for a siRNA. Here, we reported a parallel analysis of 12 pairs of antisense DNAs and siRNA duplexes for their potency to inhibit reporter luciferase activity in mammalian cells, both of the antisense DNA and siRNA agents in a pair being directed to same site in the mRNA. Five siRNAs and two antisense DNAs turned out to be effective, but the sites targeted by those effective siRNAs and antisense DNAs did not overlap. Our results indicated that effective antisense DNAs and siRNAs have different preferences for target sites in the mRNA.
Journal of General Virology | 2001
Kerstin Sollerbrant; Joacim Elmén; Claes Wahlestedt; Joel Acker; Hélène Leblois-Prehaud; Martine Latta-Mahieu; Patrice Yeh; Michel Perricaudet
The baculovirus Autographa californica multiple nucleopolyhedrosis virus causes non-productive infection in mammalian cells. Recombinant baculovirus therefore has the capability to transfer and express heterologous genes in these cells if a mammalian promoter governs the gene of interest. We have investigated the possibility of using baculovirus as a tool to produce recombinant adeno-associated virus (rAAV). AAV has become increasingly popular as a vector for gene therapy and functional genomics efforts, although its use is hampered by the lack of a simple and efficient vector production method. We show here that co-infection of mammalian producer cells with three viruses - a baculovirus containing the reporter gene flanked by AAV ITRs, a baculovirus expressing the AAV rep gene and a helper adenovirus expressing the AAV cap gene - produces infectious rAAV particles. This baculovirus-based chimeric vector method may in future improve large-scale rAAV vector preparations and circumvent present-day problems associated with rAAV production.
FEBS Letters | 2004
Joacim Elmén; Hong Yan Zhang; Bartek Zuber; Karl Ljungberg; Britta Wahren; Claes Wahlestedt; Zicai Liang
We have evaluated antisense design and efficacy of locked nucleic acid (LNA) and DNA oligonucleotide (ON) mix‐mers targeting the conserved HIV‐1 dimerization initiation site (DIS). LNA is a high affinity nucleotide analog, nuclease resistant and elicits minimal toxicity. We show that inclusion of LNA bases in antisense ONs augments the interference of HIV‐1 genome dimerization. We also demonstrate the concomitant RNase H activation by six consecutive DNA bases in an LNA/DNA mix‐mer. We show ON uptake via receptor‐mediated transfection of a human T‐cell line in which the mix‐mers subsequently inhibit replication of a clinical HIV‐1 isolate. Thus, the technique of LNA/DNA mix‐mer antisense ONs targeting the conserved HIV‐1 DIS region may provide a strategy to prevent HIV‐1 assembly in the clinic.
Nucleic Acids Research | 2005
Joacim Elmén; Håkan Thonberg; Karl Ljungberg; Miriam Frieden; Majken Westergaard; Yunhe Xu; Britta Wahren; Zicai Liang; Henrik Ørum; Troels Koch; Claes Wahlestedt
Biochemical and Biophysical Research Communications | 2004
Yunhe Xu; Annika Linde; Ola Larsson; Dorit Thormeyer; Joacim Elmén; Claes Wahlestedt; Zicai Liang
Archive | 2011
Maj Hedtjärn; Henrik Ørum; Joacim Elmén
Archive | 2004
Joacim Elmén; Claes Wahlestedt; Zicai Liang; Anders Malling Soerensen; Henrik Oerum; Troels Koch
Archive | 2004
Joacim Elmén; Claes Wahlestedt; Zicai Liang; Anders Malling Sørensen; Henrik Ørum; Troels Koch
Archive | 2004
Joacim Elmén; Claes Wahlestedt; Zicai Liang; Anders Malling Soerensen; Henrik Oerum; Troels Koch
Archive | 2004
Joacim Elmén; Claes Wahlestedt; Zicai Liang; Anders Malling Soerensen; Henrik Oerum; Troels Koch