Rescue of measles viruses from cloned DNA.

Radecke, Frank; Spielhofer, Pius; Schneider, Hans‐Jürgen; Kaelin, Karin; Huber, Marion; Dötsch, Christina; Christiansen, G.; Billeter, Martin

doi:10.1002/j.1460-2075.1995.tb00266.x

Cited by 593 publications

(621 citation statements)

References 51 publications

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“…In contrast to previous attempts with SeV and other mononegaviruses Garcin et al 1995;Lawson et al 1994;Radecke et al 1995;Schnell et al 1994;Whelan et al 1995), our system consistently recovered infectious virus even from pSeV(ÿ) that generates (ÿ)RNA (Table 1). Although the frequency was lower than that from pSeV( ) (1/50-1/100), an additional passage in eggs was sufficient to generate maximal amounts of virus (Table 1).…”

Section: Sev Recovery From Both Psev( ) and Psev(ÿ)contrasting

confidence: 92%

“…The recovery of infectious viruses from cloned and transfected cDNA will be an innovative technology, enabling the genetic engineering of viruses in this superfamily. The DNA transfection system has been established for two rhabdoviruses: rabies virus (Schnell et al 1994) and vesicular stomatitis virus (VSV) (Lawson et al 1995;Whelan et al 1995), with a genome of about 12 kilobases (kb), and for three paramyxoviruses: measles (Radecke et al 1995), Sendai (Garcin et al 1995), and RS (Collins et al 1995) viruses, with an approximate 15 kb genome. These systems, except for that of the measles virus, employed the transfection of cDNA into cells in which the cDNA and the plasmids carrying the viral nucleocapsid protein (NP or N) and RNA polymerase genes are coexpressed by vaccinia virus (VV)-driven bacteriophage T7 RNA polymerase (T7 pol).…”

Section: Introductionmentioning

confidence: 99%

“…The encapsidation in the normal virus life cycle is thought to initiate at, or very close to, the 5 0 end of the nascent RNA chain, and then to progress strictly coupled with the chain elongation under the continuous supply of NP (Lamb & Kolakofsky 1996). This highly coordinated encapsidation probably does not occur in the initial round of transcription catalysed by T7 pol, because it elongates the chain much faster than mononegavirus polymerases (Chamberlin & Ryan 1982;Iverson & Rose 1981;Radecke et al 1995). The initial transcripts could thus remain naked for some time, or sparsely bound with NP, and hence would be readily attacked by RNases (Radecke et al 1995).…”

Section: Introductionmentioning

confidence: 99%

“…This highly coordinated encapsidation probably does not occur in the initial round of transcription catalysed by T7 pol, because it elongates the chain much faster than mononegavirus polymerases (Chamberlin & Ryan 1982;Iverson & Rose 1981;Radecke et al 1995). The initial transcripts could thus remain naked for some time, or sparsely bound with NP, and hence would be readily attacked by RNases (Radecke et al 1995). Therefore, it has been presumed that the encapsidation of primary transcripts is the bottleneck in the process leading to virus recovery from cDNA.…”

Section: Introductionmentioning

confidence: 99%

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Initiation of Sendai virus multiplication from transfected cDNA or RNA with negative or positive sense

et al. 1996

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Background: The mononegavirus superfamily (Mononegavirales) comprises three families, Rhabdoviridae, Paramyxoviridae and Filoviridae. These viruses possess a single stranded negative sense RNA as the genome. Recentsuccessintherecoveryofinfectiousvirusfroma transfected cDNA of mononegaviruses including Sendai virus, a prototypic paramyxovirus, is opening the possibility of their genetic engineering. However, infectious viruses have been recovered only by initiating the infectious cycle with cDNA directing the synthesis of antigenomic positive sense ( ) RNA. Starting with genomic negative sense (ÿ) RNA has been unsuccessful. Furthermore, the recovery efficiency has often been extremely low.

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Section: Sev Recovery From Both Psev( ) and Psev(ÿ)contrasting

confidence: 92%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Initiation of Sendai virus multiplication from transfected cDNA or RNA with negative or positive sense

et al. 1996

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“…The development of systems during the last decade which permit the generation of recombinant MVs, 'virus rescue' [187], has opened the door to mechanistic studies, not only of MV persistence and its role in neurological sequelae of MV infection and the role of specific genes in this process, but also dissection of the roles of individual genes in isolation or in combination with others, in attenuation, virulence immunosuppression, and interaction with the innate immune system.…”

Section: The Value Of Animal Model Systemsmentioning

confidence: 99%

Morbilliviruses and human disease

Rima

Duprex

2005

The Journal of Pathology

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Morbilliviruses are a group of viruses that belong to the family Paramyxoviridae. The most instantly recognizable member is measles virus (MV) and individuals acutely infected with the virus exhibit a wide range of clinical symptoms ranging from a characteristic mild selflimiting infection to death. Canine distemper virus (CDV) and rinderpest virus (RPV) cause a similar but distinctive pathology in dogs and cattle, respectively, and these, alongside experimental MV infection of primates, have been useful models for MV pathogenesis. Traditionally, viruses were identified because a distinctive disease was observed in man or animals; an infectious agent was subsequently isolated, cultured, and this could be used to recapitulate the disease in an experimentally infected host. Thus, satisfying Koch's postulates has been the norm. More recently, particularly due to the advent of exceedingly sensitive molecular biological assays, many researchers have looked for infectious agents in disease conditions for which a viral aetiology has not been previously established. For these cases, the modified Koch's postulates of Bradford Hill have been developed as criteria to link a virus to a specific disease. Only in a few cases have these conditions been fulfilled. Therefore, many viruses have over the years been definitely and tentatively linked to human diseases and in this respect the morbilliviruses are no different. In this review, human diseases associated with morbillivirus infection have been grouped into three broad categories: (1) those which are definitely caused by the infection; (2) those which may be exacerbated or facilitated by an infection; and (3) those which currently have limited, weak, unsubstantiated or no credible scientific evidence to support any link to a morbillivirus. Thus, an attempt has been made to clarify the published data and separate human diseases actually linked to morbilliviruses from those that are merely anecdotally associated.

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Reverse Genetics Meets the Nonsegmented Negative-Strand RNA Viruses

Radecke

Billeter

1997

Rev. Med. Virol.

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Rescue of measles viruses from cloned DNA.

Cited by 593 publications

References 51 publications

Initiation of Sendai virus multiplication from transfected cDNA or RNA with negative or positive sense

Initiation of Sendai virus multiplication from transfected cDNA or RNA with negative or positive sense

Morbilliviruses and human disease

Reverse Genetics Meets the Nonsegmented Negative-Strand RNA Viruses

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