1.Yaws in the periurban settlements of Port Moresby, Papua New Guinea.
Laurens A Manning ; Graham D Ogle
Papua and New Guinea medical journal 2002;45(3-4):206-12
Yaws is a re-emerging disease in Papua New Guinea. A resurgence of yaws is documented in the periurban settlements around Port Moresby. A total of 494 cases were identified from April 2000 to September 2001. The age distribution ranged from 2 years to adult (median 9 years). Presenting symptoms were adequately recorded in 286 cases (58%). Of these, 42% presented with raised painless sores, 47% with bone/joint symptoms only and 11% with both sores and bone/joint symptoms. Children in communities with a suspected high prevalence were surveyed and examined for presence of primary yaws sores. 33 out of 227 children examined (15%) had evidence of primary yaws sores. Initial control measures have been case-finding and treatment of contacts, but in areas of known high prevalence mass treatment is planned.
Yaws
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Mores
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Port - alcoholic beverage
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Papua New Guinea
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joint symptom
2.Improved laboratory capacity is required to respond better to future cholera outbreaks in Papua New Guinea
Andrew Greenhill ; Alexander Rosewell ; Monalisa Kas ; Laurens Manning ; Leomeldo Latorre ; Peter Siba ; Paul Horwood
Western Pacific Surveillance and Response 2012;3(2):30-32
Cholera was first detected in Papua New Guinea in July 2009, caused by Vibrio cholerae O1 El Tor serotype Ogawa. By late 2011, 15 500 cases had been reported throughout lowland Papua New Guinea with a case fatality rate of 3.2%. The epidemic has since slowed, with only sporadic cases reported in Western Province and the Autonomous Region of Bougainville (ARB). Accurate and timely diagnosis is a critical element of the public health response to cholera, yet in low-income countries where the burden of cholera is the greatest, diagnostic services are often limited. Here we report on the diagnostic challenges and the logistical factors that impacted on diagnosis during the first reported outbreak of cholera in Papua New Guinea.
3.Bloodstream infections caused by resistant bacteria in surgical patients admitted to Modilon Hospital, Madang.
Asa, Henao ; Laman, Moses ; Greenhill, Andrew R ; Siba, Peter M ; Davis, Timothy M E ; Maihua, John ; Manning, Laurens
Papua and New Guinea medical journal 2012;55(1-4):5-11
In view of the dearth of information relating to antibiotic resistance in community- and hospital-acquired bacterial infections in Papua New Guinea (PNG), we carried out a prospective, hospital-based observational study of surgical patients between October 2008 and October 2009. In a sample of 115 patients (median age 30 years; 55% males) suspected of having a bloodstream infection, blood cultures were positive in 11 (10%) and a significant pathogen was isolated in 9 (8%). Staphylococcus aureus was isolated in 4 patients (44%) and 3 were methicillin resistant; all these isolates were considered community acquired because cultures were performed within 48 hours of admission. Of the remaining 5 isolates, 4 were Gram-negative organisms with at least intermediate resistance to chloramphenicol that were grown from blood taken > 48 hours post-admission and thus considered nosocomially acquired. These data suggest two distinct patterns of bacterial infection in PNG surgical inpatients that have implications for national antibiotic prescription guidelines.
4. Investigation of polymorphisms in Plasmodium falciparum hrp2, hrp3, aldolase and pldh genes and their impact on the performance of malaria rapid diagnostic tests in Papua New Guinea
Elisheba Malau ; Moses Laman ; Laurens Manning ; Timothy M.E. Davis ; Peter Siba ; Alyssa Barry ; Ivo Mueller ; Celine Barnadas
Papua New Guinea medical journal 2018;61(1-4):33-45
The World Health Organization (WHO) recommends that parasitological confirmation of clinical malaria diagnosis be performed before antimalarial treatment is administered. Malaria rapid diagnostic tests (RDTs) represent a valuable tool for prompt and efficient diagnosis of malaria in settings where microscopic diagnosis is unavailable or unreliable. Concerns remain, however, that Plasmodium falciparum polymorphisms in the genes coding the antigens detected by RDT could impact on RDT performance. Using field isolates of Plasmodium falciparum, we aimed to characterize genetic variability in histidine-rich proteins 2 and 3 (PfHRP-2 and PfHRP-3), aldolase (ALD) and Plasmodium lactate dehydrogenase (pLDH) genes and to evaluate their impact on the performance of RDT. Pfhrp-2, Pfhrp-3, aldolase and pldh were amplified using polymerase chain reaction (PCR) and sequenced. Genetic variation was observed in pfhrp-2 and pfhrp-3 genes while aldolase and pldh showed high levels of conservation. These findings suggest that RDTs based on pLDH and ALD are reliable in the study settings where there is intense diversity or polymorphisms of histidine-rich protein (HRP). Nevertheless, there is no evidence from this study to suggest that RDTs based on the detection of PfHRP-2 and PfHRP-3 have lower sensitivity in Papua New Guinea (PNG). The results observed in this study will be used to inform the PNG National Department of Health on the continued usage of pLDH/ HRP-2 RDT for malaria diagnosis in PNG.
5.Quality microbiological diagnostics and antimicrobial susceptibility testing, an essential component of antimicrobial resistance surveillance and control efforts in Pacific island nations
John Kenneth Ferguson ; Jacklyn Joseph ; Samson Kangapu ; Hilda Zoleveke ; Nicola Townell ; Trevor Duke ; Laurens Manning ; Evelyn Lavu
Western Pacific Surveillance and Response 2020;11(1):41-46
Problem:
Emerging bacterial antimicrobial (antibiotic) resistance (AMR) is a global threat to human health. However,
a majority of lower income countries do not have microbiological diagnostic testing for prompt, reliable confirmation of
bloodstream infection and identification of AMR.
Context:
Clinicians in Pacific island nations are increasingly challenged by patients who have infection due to antimicrobialresistant
bacteria. Treatment of infection remains empirical because of a lack of diagnostic testing capacity and may follow
guidelines that were formulated without reference to local measures of AMR prevalence. There is limited understanding
among clinicians of microbiology testing and test interpretation.
Action:
Examine the lessons learnt from pilot laboratory development programmes in two Pacific island nations that
focused on establishing standard procedures for micrological diagnostics and antimicrobial susceptibility testing (AST) and
on improving the training of clinicians to increase their use of laboratory services.
Outcome:
The pilot programmes addressed a range of logistical difficulties and evaluated two blood culture systems. They
also examined and improved internal QC implementation and evaluated the prevalence of AMR.
Discussion
Continued development of microbiological diagnostic capability in the Pacific region is paramount. Pacific
Island nations need to develop the capability of at least one central laboratory to culture AMR pathogens and subject them
to quality-controlled AST or arrange for suitable referral to a nearby country.