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Volume 19, Number 12—December 2013
Letter

Treponemal Infection in Nonhuman Primates as Possible Reservoir for Human Yaws

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To the Editor: In 2012, the World Health Organization launched plans for a second campaign to eradicate the neglected tropical disease, yaws (1). The first campaign, conducted during the mid-20th century, was tremendously successful in terms of treatment and reduced the number of cases by 95%. However, it failed to eradicate the disease, and when local efforts to prevent new cases proved insufficient, yaws resurged in some areas. Comments on the new yaws eradication campaign have emphasized the need for sustained support and resources. Here we draw attention to an additional concern that could impede yaws eradication efforts.

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Thumbnail of Geographic proximity between human yaws and endemic syphilis, as estimated by the World Health Organization, and locations in which treponemal infection has been identified in nonhuman primates (NHPs), Africa, 1990s. Red dots indicate infection in NHPs confirmed by sensitive and specific treponemal serologic tests (TPI/FTA-ABS/MHA-TP [Treponema-pallidum-immobilization reaction/fluorescence-Treponema-antibody-absorption test/Treponema pallidum microhemagglutination assay]) and, in so

Figure. . Geographic proximity between human yaws and endemic syphilis, as estimated by the World Health Organization, and locations in which treponemal infection has been identified in nonhuman primates (NHPs), Africa, 1990s....

The success of any eradication campaign depends on the absence of a nonhuman reservoir. Smallpox had no known animal reservoir, and polio and dracunculiasis (guinea worm disease), which are currently the focus of the World Health Organization eradication campaigns, also have none. By contrast, compelling evidence suggests that yaws exists in wild nonhuman primate populations residing in regions where humans are also infected (Figure).

The subspecies of the bacterium Treponema pallidum that cause the non–sexually transmitted diseases yaws (subsp. pertenue infection) and endemic syphilis (subsp. endemicum infection) and the sexually transmitted infection syphilis (subsp. pallidum) are close relatives. The 3 diseases cannot be distinguished serologically. Instead, the diseases they cause are usually differentiated by clinical characteristics and geographic distribution. Whereas syphilis is a venereal disease with a worldwide distribution, yaws primarily affects children in hot and humid areas of Africa and Asia, and endemic syphilis occurs in arid regions. Because methods available to differentiate between the T. pallidum subspecies were unavailable in the past, prevalence data for yaws were sometimes vague and inaccurate. Recently, molecular tests capable of distinguishing between the subspecies by using single nucleotide polymorphisms have been developed (2,3). These tests have enabled us to learn more about the T. pallidum strains that infect wild nonhuman primates.

During the 1960s, researchers reported that many baboons in West Africa were seropositive for treponemal infection (4). Since then, high levels of infection have been documented in other monkey species in West Africa and in great apes (5). Recently, we documented T. pallidum infection in olive baboons (Papio anubis) at Lake Manyara National Park in Tanzania (6). In West Africa, clinical signs of infection in nonhuman primates are usually mild, if present at all, consisting of small lesions around the muzzle, eyelids, and armpits (4). A recent survey in 2013 at Parc National du Niokolo-Koba, Senegal, revealed T. pallidum antibodies in Guinea baboons (P. papio) with no signs of infection (S. Knauf et al, unpub. data). By contrast, severe manifestations resembling tertiary-stage yaws have been reported in wild gorillas (5). In terms of genetic distance, studies thus far indicate that the organisms infecting baboons in West and East Africa closely resemble T. pallidum subsp. pertenue, the agent responsible for yaws in humans (2,7). In fact, the genome sequence of a T. pallidum strain collected from a baboon in Guinea indicates that it should be considered a T. pallidum subsp. pertenue strain (8). Infection has been confirmed by serologic tests in a variety of nonhuman primate species in the yaws belt of Africa and by PCR in baboons from East and West Africa (Figure).

The high prevalence of nonhuman primate infection in areas of tropical Africa where yaws is common in humans (Figure) suggests that cross-species infection may occur. Decades ago, researchers reported that the Fribourg-Blanc simian strain, collected in Guinea, can cause sustained infection in humans after inoculation (9). Such experiments are ethically questionable and the details given are scant, but this work suggests that simian strains have zoonotic potential. Additional research is needed to determine whether interspecies transmission of T. pallidum occurs under natural conditions. Bush meat preparation is common in many African countries and a major source of zoonotic infection. It involves frequent skin-to-skin contact, which is the preferred mode of transmission for yaws. Insects also have been proposed to be vectors of infection, although this has not been documented (10). If evidence of interspecies yaws transmission, either direct or by vector, is discovered, then nonhuman primates may be a major reservoir of infection for humans.

Additional studies comparing human and simian strains may show whether zoonotic transmission of T. pallidum occurs frequently, an important consideration with regard to disease eradication and the conservation of great apes and other endangered nonhuman primates. To eradicate yaws, all host species and any possible reservoirs need to be taken into account. We, like the rest of the world, want the second yaws eradication campaign to succeed and hope that nonhuman primate infection will be evaluated as a factor in disease transmission.

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Sascha KnaufComments to Author , Hsi Liu, and Kristin N. Harper
Author affiliations: German Primate Center, Göttingen, Germany (S. Knauf); Centers for Diseases Control and Prevention, Atlanta, Georgia, USA (H. Liu); Columbia University Medical Center, New York, New York, USA (K.N. Harper)

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References

  1. Maurice  J. WHO plans new yaws eradication campaign. Lancet. 2012;379:13778. DOIPubMedGoogle Scholar
  2. Harper  KN, Ocampo  PS, Steiner  BM, George  RW, Silverman  MS, Bolotin  S, On the origin of the treponematoses: a phylogenetic approach. PLoS Negl Trop Dis. 2008;2:e148. DOIPubMedGoogle Scholar
  3. Centurion-Lara  A, Castro  C, Castillo  R, Shaffer  J. Voorhis Wv, Lukehart S. The flanking region sequences of the 15-kDa lipoprotein gene differentiate pathogenic treponemes. J Infect Dis. 1998;177:103640. DOIPubMedGoogle Scholar
  4. Fribourg-Blanc  A, Mollaret  HH. Natural treponematosis of the African primate. Primates Med. 1969;3:11321 .PubMedGoogle Scholar
  5. Levréro  F, Gatti  S, Gautier-Hion  A, Ménard  N. Yaws disease in a wild gorilla population and its impact on the reproductive status of males. Am J Phys Anthropol. 2007;132:56875. DOIPubMedGoogle Scholar
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  7. Harper  KN, Fyumagwa  R, Hoare  R, Wambura  P, Coppenhaver  D, Sapolsky  R, Treponema pallidum infection in the wild baboons of East Africa: distribution and genetic characterization of the strains responsible. PLoS ONE. 2012;7:e50882. DOIPubMedGoogle Scholar
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  9. Smith  JL, David  NJ, Indgin  S, Israel  CW, Levine  BM, Justice  J Jr, Neuro-ophthalmological study of late yaws and pinta. II. The Caracas project. Br J Vener Dis. 1971;47:22651 .PubMedGoogle Scholar
  10. Thomson  JG, Lamborn  WA. Mechanical transmission of trypanosomiasis, leishmaniasis, and yaws through the agency of non-biting haematophagous flies. BMJ. 1934;2:5069. DOIPubMedGoogle Scholar

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DOI: 10.3201/eid1912.130863

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Sascha Knauf, Pathology Unit, German Primate Center, Kellnerweg 4, 37077 Göttingen, GermanySascha Knauf, Pathology Unit, German Primate Center, Kellnerweg 4, 37077 Göttingen, Germany

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Page created: November 20, 2013
Page updated: November 20, 2013
Page reviewed: November 20, 2013
The conclusions, findings, and opinions expressed by authors contributing to this journal do not necessarily reflect the official position of the U.S. Department of Health and Human Services, the Public Health Service, the Centers for Disease Control and Prevention, or the authors' affiliated institutions. Use of trade names is for identification only and does not imply endorsement by any of the groups named above.
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