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Novel measles virus genotype, East Timor and Australia. (Dispatches).


Measles outbreaks in 1999 in Queensland and Victoria, Australia, were caused by a novel strain of clade clade Cladus, subtype Genetics A branch of biological taxa or species that share features inherited from a common ancestor; a single phylogenetic group or line. See Inheritance, Species.  G virus (proposed name g3). Epidemiologic and molecular evidence supports independent circulation of this virus in Queensland, northern Australia The term northern Australia is generally considered to include the States and territories of Australia of Queensland and the Northern Territory. The part of Western Australia (WA) north of latitude 26° south — a definition widely used in law and State government policy , in addition to importation of the virus by East Timor East Timor (tē`môr) or Timor-Leste (–lĕsht), Tetum Timor Lorosae, republic, officially Democratic Republic of Timor-Leste (2002 est. pop.  refugees seeking safe haven 1. Designated area(s) to which noncombatants of the United States Government's responsibility and commercial vehicles and materiel may be evacuated during a domestic or other valid emergency.
2.
 in Australia.

**********

Strategies to reduce Measles virus measles virus
n.
An RNA virus of the genus Morbillivirus that causes measles in humans. Also called rubeola virus.
 (MeV) circulation in industrialized in·dus·tri·al·ize  
v. in·dus·tri·al·ized, in·dus·tri·al·iz·ing, in·dus·tri·al·iz·es

v.tr.
1. To develop industry in (a country or society, for example).

2.
 countries, such as aggressive vaccination campaigns targeting children, have proven successful (1). Nevertheless, through introduction from other geographic locations, the virus continues to cause outbreaks in industrialized countries in unvaccinated persons.

In Victoria, measles is a reportable disease re·port·a·ble disease
n.
See notifiable disease.
, and an enhanced surveillance strategy has been operational since 1997. A registered nurse visits the homes of patients with reported cases to collect specimens for laboratory confirmation, by polymerase chain reaction polymerase chain reaction (pŏl`ĭmərās') (PCR), laboratory process in which a particular DNA segment from a mixture of DNA chains is rapidly replicated, producing a large, readily analyzed sample of a piece of DNA; the process is  or detection of MeV-specific immunoglobulin (Ig) M, of the clinical diagnosis and subsequent identification of the measles genotype (2). For other Australian states, specimens from laboratory-confirmed cases are sent for genotyping to the WHO regional measles reference laboratory for the western Pacific Region.

Variable regions in the MeV genome include the hemagglutinin hemagglutinin /he·mag·glu·ti·nin/ (-gloo´ti-nin) an antibody that causes agglutination of erythrocytes.

cold hemagglutinin  one which acts only at temperatures near 4° C.
 (H) and nucleoprotein nucleoprotein

Macromolecular complex consisting of a protein linked to a nucleic acid, either DNA or RNA. The proteins that combine with DNA are generally of characteristic types called histones and protamines.
 (N) genes. The most variable region is the carboxyl-terminal end (450 nucleotides [nt]) of the N gene. A uniform nomenclature approved by World Health Organization (WHO) has existed since 1998 and is used in classifying and naming measles viruses. Currently, 20 genotypes and 1 proposed new genotype exist, encompassing eight clades designated A-H. Each clade contains MeV genotypes that are related by [greater than or equal to] 2.5% nt divergence in the 450-bp carboxyl-terminal end of the N gene and 2% in the H gene (3). Clades are distinguished by greater nucleotide differences, location of nucleotides, and specific nucleotides shared in genotypes of a particular clade.

Until recently, MeV strains belonging to clade G had not been detected for >15 years, and the lineage was considered to be either extinct or inactive (4). However, retrospective sequence analysis of a measles strain isolated from an immunocompromised immunocompromised /im·mu·no·com·pro·mised/ (-kom´pro-mizd) having the immune response attenuated by administration of immunosuppressive drugs, by irradiation, by malnutrition, or by certain disease processes (e.g., cancer).  infant from the Netherlands, who had been infected in Indonesia in 1997, and of measles strains associated with outbreaks in Indonesia and Malaysia in 1999 have demonstrated that this genotype has circulated in the intervening period (5-6). We describe the circulation of a novel genotype of MeV in Australia and investigate its likely origin.

The Study

In June 1999, the novel genotype was first identified in Victoria in a 24-year-old Australian man who had symptoms of MeV infection shortly after visiting the northern state of Queensland. In the next 2 months, four more cases of infection with the same genotype were identified in Queensland. Epidemiologic links between these five cases could not be established.

In the second week of September 1999, refugees from the newly independent country of East Timor arrived in Darwin, Northern Territory “Port Darwin” redirects here. For the old name of Falkland Islands, see Darwin, Falkland Islands.

Darwin is the capital city of the Australian Territory of the Northern Territory.
, where they underwent preliminary medical examinations before being moved to a safe-haven refugee camp in regional Victoria. Several days after arriving at the safe haven, a 4-year-old girl had symptoms that matched the clinical case definition of measles infection (rash and cough with fever at onset of rash) (7). The diagnosis was confirmed serologically with an Enzygnost Anti-measles-virus/IgM kit (Dade Behring, Marburg, Germany). Active surveillance of all contacts of the initial patient and all residents reporting to the safe-haven medical center with symptoms suggestive of suggestive of Decision making adjective Referring to a pattern by LM or imaging, that the interpreter associates with a particular–usually malignant lesion. See Aunt Millie approach, Defensive medicine.  measles infection identified 11 other cases (4 laboratory confirmed) in children <13 years of age in the safe haven; a 26-year-old volunteer worker who worked at the accident and emergency department of the same hospital that admitted some of the infected refugees was also diagnosed with measles infection. Subsequent molecular analysis confirmed the volunteer's infection as being caused by the same virus as the refugees. The last recognized case of this MeV genotype occurred in early November 1999, when a United Nations International Force East Timor (Interfet) soldier, who showed clinical symptoms in East Timor immediately before he was transferred to Darwin, was confirmed as being infected with MeV.

The commonality of the virus strains circulating in both Australia and East Timor was confirmed through analysis of MeV RNA RNA: see nucleic acid.
RNA
 in full ribonucleic acid

One of the two main types of nucleic acid (the other being DNA), which functions in cellular protein synthesis in all living cells and replaces DNA as the carrier of genetic
 (8). Analysis of the 456-bp carboxyl-terminal region of the N gene of the Victorian and Queensland samples yielded identical sequences in most cases, suggesting that these patients were infected with the same strain of MeV as the East Timorese. Nevertheless, no epidemiologic links were apparent between the Queensland cases and the subsequent cases in East Timorese refugees.

The N gene sequences of measles viruses identified from June to November 1999 were most closely related to the Amsterdam prototype G2 strain identified by de Swart swart  
adj. Archaic
Swarthy.



[Middle English swarte, from Old English sweart.]

Adj. 1.
 et al. (4). Although phylogenetic phy·lo·ge·net·ic
adj.
1. Of or relating to phylogeny or phylogenetics.

2. Relating to or based on evolutionary development or history.
 analysis indicated that these sequences belonged within the clade G viruses, they differed from the G2 prototype strain by 12 (2.6%) nt and by deduction 6 (4%) amino acids (Figure). N gene sequences were obtained from 17 clinical samples. As a group, these 17 samples shared an amino acid (439K) in the N protein not previously seen in any other reference prototypes analyzed. Thirteen of these samples were identical in sequence (samples 1-13, Table). Three samples (samples 14-16, Table) differed by a single nucleotide, which resulted in another novel amino acid change, P456L. One sample (sample 17, Table) diverged by 2 nt, one silent and the other resulting in the same P456L change seen in samples 14-16. Differences seen in these 17 samples did not appear to be related to the geographic location of the cases.

[FIGURE OMITTED]

Full or partial H gene sequences were derived from the measles viruses of four samples obtained from patients 8, 13, 15, and 16. Phylogenetic analysis of the H gene of the first 842 nt of these samples confirmed their assignment to the clade G viruses (results not shown). The four sequences analyzed showed up to 1.1% intranucleotide divergence. The MeV from patient 8 varied by 2.1% nt sequence compared with the prototype G2 strain. Comparison of nucleotide and amino acid sequence of the H gene of the one sample (from patient 13) with full H gene sequence showed differences from the prototype G2 strain of 35 (1.9%) nt and 13 (2.1%) amino acids. This sequence also contained amino acids in the H protein not previously found in other reference prototypes, namely 212Q, 225H, 238D, and 495N. Phylogenetic analysis of the full H gene sequence showed similar patterns of relatedness to those obtained for the N gene (results not shown).

Together, phylogenetic analysis of the N and H genes and the appearance of novel amino acids in the H protein provided strong evidence that these measles virus were sufficiently unrelated to the prototype G2 strain to enable their classification as a new genotype within clade G. We propose that measles virus/Vic.AU/24.99 be the reference sequence for a new genotype, g3, pending isolation of a reference strain (3). Gen-Bank accession numbers for the 456-bp carboxyl-terminal end of three of the N gene sequences are shown in the Table. The GenBank accession number for the full-length H gene is AF35362.

The novel g3 MeV was not the only strain circulating in Australia during this time. Coinciding with the genotype g3 outbreak, four cases of genotype D8 were identified in Victoria. Three months earlier, small clusters of measles cases were identified in two other Australian states, genotype D5 in the Northern Territory and genotype D3 in Western Australia Western Australia, state (1991 pop. 1,409,965), 975,920 sq mi (2,527,633 sq km), Australia, comprising the entire western part of the continent. It is bounded on the N, W, and S by the Indian Ocean. Perth is the capital. . Soon after the g3 outbreak, genotype D7 circulated in Victoria, Queensland, and the Northern Territory.

In recent years, vaccination campaigns have been undertaken in East Timor under the guidance of United Nations Children's Fund United Nations Children's Fund (UNICEF), an affiliated agency of the United Nations. It was established in 1946 as the United Nations International Children's Emergency Fund.  (UNICEF UNICEF (y`nĭsĕf'), the United Nations Children's Fund, an affiliated agency of the United Nations. ) and WHO. In October 1999, UNICEF conducted a major immunization immunization: see immunity; vaccination.  campaign in Dili, East Timor, reaching approximately 4,000 children <5 years of age; in March 2000, >45,000 children were vaccinated (9). Nevertheless, from January 2000 to May 2001, a total of 1,479 cases of suspected measles infection were reported in East Timor.

In an industrialized country like Australia, where no apparent circulation of an indigenous MeV strain occurs, the use of epidemiologic surveillance epidemiologic surveillance The ongoing, systematic collection, analysis, and interpretation of health data essential to planning, implementing, and evaluating public health practice, closely integrated with the timely dissemination of these data to those who need to know  and molecular characterization is important in tracing the source and transmission pathways of MeV imported from areas where the disease is endemic. Apart from expanding our global knowledge of MeV genotypes, molecular characterization is also useful in clarifying epidemiologic links and distinguishing between vaccine-associated and wild-type infection.

Despite the novelty of the circulating MeV genotypes, our findings highlight the need for continued vigilance if the virus is to be eradicated. The humanitarian movement of refugees from a country where MeV infection is uncontrolled to countries with relatively high MeV herd immunity herd immunity
n.
1. Resistance to the spread of infectious disease in a group because susceptible members are few, making transmission from an infected member unlikely.

2.
 is now a common occurrence. Thus, the potential for transmission of this highly infectious virus to residual susceptibles in the wider community remains a distinct possibility, as demonstrated by this outbreak. Measures, such as vaccination of military personnel and support staff working directly with displaced persons; use of appropriate infection-control procedures when attending sick refugees; and screening of newly arrived refugees from measles-endemic areas, are likely to decrease transmission of MeV in industrialized countries.
Table. Unique predicted amino acid differences compared with all
reference measles virus sequences in 456-bp carboxyl-terminal end
of N (a) gene (b)

Sample no.    Predicted amino acid differences    Accession no.

1-13                      439K (c)                  AF353622
14-16                  439K (c); 456L               AY055850
17                     439K (c); 456L               AY055851

(a) N, nucleoprotein.

(b) Identified from 17 clinical samples in the outbreak.

(c) Unique to proposed genotype g3.


Acknowledgments

We thank Stephen Lambert Stephen Lambert (born December 21, 1979) is a field hockey goalkeeper from Australia, who was first selected to play for The Kookaburras at the Four Nations International Challenge in June 2002. , David Smith, and Robyn Wood for their assistance with provision of clinical material and epidemiologic information.

References

(1.) World Health Organization. Measles. Progress towards global control and regional elimination 1998-1999. Wkly Epidemiol Rec 1999;74:429-40.

(2.) The Enhanced Measles Surveillance Working Party. Implementing a system of enhanced surveillance for measles in Victoria. Commun Dis Intell 1999;23:51-4.

(3.) World Health Organization. Nomenclature for describing the genetic characteristics of wild-type measles viruses. Wkly Epidemiol Rec 2001;76:242-7.

(4.) World Health Organization. Expanded programme on immunization--standardization of the nomenclature for describing the genetic characteristics of wild-type measles viruses. Wkly Epidemiol Rec 1998;73:265-9.

(5.) de Swart RL, Wertheim-van Dillen PME PME Petites et Moyennes Entreprises
PME Professional Military Education
PME Pequenas e Médias Empresas (Portugal)
PME Petite et Moyenne Entreprise
PME Psychology of Mathematics Education
PME Pi Mu Epsilon
, van Binnendijk RS, Muller CP, Frenkel J, Osterhaus ADME ADME Absorption, Distribution, Metabolism, and Excretion
ADME Association of Destination Management Executives
ADME Active Duty Medical Extension
. Measles in a Dutch hospital introduced by an immuno-compromised infant from Indonesia infected with a new virus genotype. Lancet 2000;355:201-2.

(6.) Rota PA, Liffick S, Rosenthal S, Heriyanto B, Chua KB. Measles genotype G2 in Indonesia and Malaysia. Lancet 2000;355:1557-8.

(7.) Ferson MJ, Young LC, Robertson PW, Whybin LR. Difficulties in clinical diagnosis of measles: proposal for a modified case definition. Med J Aust 1995;163:364-6.

(8.) Chibo D, Birch CJ, Rota PA, Catton MG. Molecular characterization of measles viruses isolated in Victoria, Australia, between 1973 and 1998. J Gen Virol 2000;81:2511-8.

(9.) World Health Organization. Background paper for Donors' Meeting on East Timor. Canberra, 14-15 June 2001. Dili, East Timor. World Health Organization; 2001. Available from: URL URL
 in full Uniform Resource Locator

Address of a resource on the Internet. The resource can be any type of file stored on a server, such as a Web page, a text file, a graphics file, or an application program.
: http://www.who.int/disasters/ repo/6979.doc

Ms. Chibo is a medical scientist at the Victorian Infectious Diseases Reference Laboratory in Victoria, Australia. Her main interests are the use of molecular techniques and phylogenetic analysis to study viruses of public health importance and mechanisms associated with development of resistance to antiviral drugs Antiviral Drugs Definition

Antiviral drugs are medicines that cure or control virus infections.
Purpose

Antivirals are used to treat infections caused by viruses.
 by herpesviruses Herpesviruses
A family of viruses responsible for cold sores, chicken pox, and genital herpes.

Mentioned in: Skin Resurfacing
.

Doris Chibo, * Michaela Riddell, * Michael Catton, * and Christopher Birch *

* World Health Organization Regional Measles Reference Laboratory for the Western Pacific Region, North Melbourne, Victoria This article is about a Suburb in Melbourne; the name may also refer to the North Melbourne Football Club.

North Melbourne is a suburb of Melbourne, Australia in the state of Victoria. It is in the Local Government Area of the City of Melbourne.
, Australia

Address for correspondence: Christopher Birch, 10 Wreckyn St., North Melbourne 3051, Victoria, Australia; fax: 61 3 9342 2666; e-mail: chris.birch@mh.org.au
COPYRIGHT 2002 U.S. National Center for Infectious Diseases
No portion of this article can be reproduced without the express written permission from the copyright holder.
Copyright 2002, Gale Group. All rights reserved. Gale Group is a Thomson Corporation Company.

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Author:Birch, Christopher
Publication:Emerging Infectious Diseases
Date:Jul 1, 2002
Words:1924
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