In Alberta, the first case of congenital syphilis in over 10 years was reported in 2002. This was after a resurgence in the province in 2000 of locally acquired infectious syphilis, in many cases affecting people who reported casual or anonymous sexual partnering.
In 1996, Canada set a goal to maintain the rate of infectious syphilis at no more than 0.5 per 100 000 population.1 At that time, the elimination of syphilis in Canada seemed achievable.2
However, the following year (mid-1997), an outbreak of infectious syphilis was reported in downtown Vancouver.3 Between 1996 and 2006, Alberta experienced a progressive rise in cases of infectious syphilis, from 0 in 1996 to 6.5 per 100 000 in 2006. In the northern part of the province, this outbreak has involved mostly heterosexual people, but in the south, it affects mainly men who have sex with men.
Syphilis serology is routinely performed for all pregnant women who obtain antenatal care in Alberta. In 2006, 50 of 55 723 prenatal tests were reactive by rapid plasma reagin, with 12 confirmed infectious and 18 confirmed noninfectious cases after individual case review (20 cases were previously treated or false positive). During 2005 and 2006, a total of 9 babies were born in Alberta with congenital syphilis; the neonatal and maternal characteristics in these cases are outlined in Table 1 and Table 2. Six of the 9 mothers were First Nations women. None of them were coinfected with HIV at the time of diagnosis; preliminary reports indicate that in the rest of Canada, there were 3 cases in 2005 and 4 cases in 2006.4
In 4 of the 9 Alberta cases of congenital syphilis, the mother did not obtain antenatal care before the onset of labour. In 1 case, the mother tested positive for syphilis but could not be located for several weeks.
In the remaining 4 cases, the mothers tested negative earlier in the pregnancy but acquired the infection later. Although 2 of these mothers had the classic genital ulcers of primary syphilis within 1 month before delivery, syphilis had not initially been considered as the cause. One mother had begun antiviral therapy for an incorrect diagnosis of genital herpes and underwent an elective cesarean section.
One baby, born late in 2006, was brought to hospital at 3 months of age with severe desquamating skin rash, massive hepatosplenomegaly, hyponatremia and anemia. Earlier in the pregnancy, the mother's syphilis serology had been reported as nonreactive; she had been married for 15 years. Her secondary syphilis was diagnosed subsequent to confirmation of the infant's infection. For this baby and for the most recently treated baby (whose diagnosis was made at 8 months of age), the initial diagnosis was juvenile myelomonocytic leukemia, on the basis of their presentation with hepatosplenomegaly, desquamating rash and anemia.
The Canadian Guidelines on Sexually Transmitted Infections4 currently recommend repeat testing for syphilis for women who remain at high risk for this disease during pregnancy (Box 1). The syphilis chapter of the guidelines will soon be revised to include, in addition to the criteria given in Box 1, recommendations for rescreening women who reside in areas where syphilis outbreaks are affecting heterosexual people. Of note, the diagnosis of congenital syphilis in the 2 babies described in the preceding paragraph was delayed because their mothers did not meet criteria for rescreening for syphilis during pregnancy, since their husbands' extramarital activities were unknown at the time of delivery.
Risk of transmission from mother to child
Transmission of syphilis to a fetus depends largely on the duration of the disease in the mother.5 The longer the interval between infection and pregnancy, the more benign the outcome in the infant (Kassowitz's law).6 The risk of transmission is 70%–100% in women with primary or secondary syphilis, 40% with early latent syphilis and 10% in late latent cases.7 About 40% of pregnancies in women with infectious syphilis result in the death of the fetus.8 Spirochetes can cross the placenta and infect the fetus at as early as 9 weeks of gestation, with the risk of fetal infection increasing with gestational age.9 The clinical spectrum in surviving infants ranges from a complete lack of symptoms to severe clinical manifestations.
Screening and rescreening of pregnant women and newborns
Routine screening during pregnancy for syphilis remains the standard of care for women in Canada. Box 1 lists the criteria for everyone at risk for syphilis. Pregnant women with these characteristics and those from geographic areas with an outbreak of infectious syphilis should be rescreened for syphilis at 28–32 weeks and again at the time of delivery. In addition to these criteria, Aboriginal women should be rescreened in geographic areas experiencing outbreaks affecting Aboriginal communities.
Women newly infected with syphilis may not be aware of symptoms, particularly if their ulcers are painless and on the internal genital tract.
All women testing positive for syphilis should also be screened for HIV; coinfection with HIV affects immediate medical management and the duration of follow-up. Because people infected with syphilis are at increased risk of HIV infection, and in light of the window period (tests for HIV antibodies tend not to show positivity until at least 4 weeks after transmission), HIV serology should also be repeated later in pregnancy. Other sexually transmitted infections (e.g., gonorrhea, chlamydia) should be tested for in all cases, with screening tests for hepatitis B and C as indicated. All genital ulcers should be tested for herpes simplex virus as well. Criteria for screening and evaluation for neonatal or early congenital syphilis are listed in Box 2. No infant should leave a hospital without the mother having been tested for syphilis at least once during pregnancy.
Management
Mothers diagnosed with infectious syphilis should be treated with the appropriate dose of benzathine penicillin G according to their stage of syphilis infection and the presence or absence of HIV coinfection. Despite the administration of a single-dose penicillin regimen, as many as 14% of women with secondary syphilis in late pregnancy will undergo a fetal death or deliver infants with clinical evidence of congenital syphilis.10–12 Some specialists recommend that any pregnant woman with infectious syphilis receive 2 doses of 2.4 million units of benzathine penicillin G, administered 1 week apart, although the efficacy of this regimen in preventing fetal syphilis is as yet unknown.13,14 It is also essential that all sexual partners be tested and treated for syphilis concurrently, to prevent reinfection of the mother.
At the present time, benzathine penicillin G is not manufactured in Canada and is available only through provincial or territorial sexually transmitted disease services, who obtain the drug through Health Canada's Special Access Programme. This long-acting preparation achieves detectable serum levels of penicillin for 2–4 weeks in nonpregnant adults, and is required for treatment of infectious syphilis to be successful; short-acting penicillin agents are inadequate to achieve a cure.15
There is no satisfactory alternative to penicillin for the treatment of syphilis during pregnancy. Data on the use of ceftriaxone are not yet sufficient; erythromycin does not penetrate the placental barrier well.16,17 Women with a history of allergy to penicillin should be desensitized and then treated with penicillin.18 A Jarisch–Herxheimer reaction (in response to the rapid death of infectious organisms) during the first 24 hours after treatment may precipitate premature labour or fetal distress; any pregnant woman being treated should be advised to seek immediate medical attention if she experiences contractions or perceives reduced fetal movement.
In the second half of pregnancy (≥ 20 weeks), women with syphilis should be managed with detailed ultrasonographic assessments in conjunction with a maternal–fetal medicine specialist. If abnormalities such as hepatomegaly, ascites, hydrops or placental thickening are present, the mother should be admitted for treatment and observation.19 The ultrasound should be used as a tool to “stage” the extent of fetal disease during the second half of pregnancy.
Close follow-up of mother and fetus is necessary after treatment, with serologic testing appropriate to the stage of infection. In women at high risk for reinfection, monthly syphilis testing may be indicated.
When infants born to mothers with infectious syphilis are evaluated, a venous sample should be obtained from both mother and baby (cord blood is unsuitable) for treponemal and nontreponemal serology. The interpretation of a neonate's reactive antibodies must take maternal history into consideration, including her stage of syphilis, treatment history and syphilis serology results. Samples of placenta, neonatal nasal discharge or skin lesions should be examined by dark-field microscopy, direct or indirect immunofluorescence assay, or polymerase chain reaction for Treponema pallidum. In addition, all infants with suspected congenital syphilis should undergo lumbar puncture for cerebrospinal fluid and long-bone radiography. Ideally, all such infants should be managed by or in conjunction with a pediatric infectious diseases specialist.
Infants should be treated at birth with crystalline penicillin G for 10 days if (1) they are symptomatic; (2) their rapid plasma reagin result is fourfold (2 tubes) as high as the mother's; (3) maternal treatment was inadequate, did not contain penicillin, is unknown or occurred during the last month of pregnancy; or (4) the maternal serologic response is inadequate and/or adequate follow-up of the infant cannot be ensured. Some experts recommend that a single intramuscular dose of 50 000 units/kg of benzathine penicillin G be given to infants born to mothers with infectious syphilis who can be confirmed to have had adequate treatment; where there is no concern about maternal reinfection; and when clinical and laboratory examination in the infant are normal.14 However, there are few data to support this approach.
Follow-up serologic testing of newborns should be performed at regular intervals.20 If the infant was not infected, rapid plasma reagin titres should decline by 3 months of age and be nonreactive by 6 months. If a child's titres are stable or increase after 6–12 months of age, he or she should be evaluated (including CSF examination) and treated for congenital syphilis. Treponemal antibodies passively transferred from the mother can be present in an infant for as long as 15 months; a reactive treponemal antibody test after 18 months of age is diagnostic for congenital syphilis.
Conclusions
Given the resurgence of congenital syphilis in Alberta, continued screening of all pregnant women for syphilis is vital. It is important to rescreen high-risk mothers and those living in areas experiencing heterosexual outbreaks of syphilis at 28–32 weeks' pregnancy and again at delivery. All infected mothers should be treated with appropriate penicillin regimens and managed in conjunction with a specialist in maternal–fetal medicine. Clinicians should have a high index of suspicion for congenital syphilis and screen neonates presenting with signs compatible with congenital syphilis, as well as asymptomatic infants in select circumstances. All infants born to mothers with infectious syphilis should receive intensive clinical and laboratory follow-up in conjunction with a pediatric specialist.
To further limit the devastating consequences of congenital syphilis, additional research and enhancement of public health capacity are necessary to develop strategies for the primary prevention of syphilis, improvements in access to prenatal care by high-risk and vulnerable populations, and assessment of sexual partners' risk factors for syphilis. Finally, it will be important to raise public and provider awareness of the resurgence of this ancient disease. Appropriate strategies to achieve this goal include communication efforts (such as mass mailings) to alert clinicians to the resurgence of syphilis and to encourage increased screening of those at risk. Other strategies might include heightening media awareness by way of press releases; disseminating information through newspaper, radio and television announcements; and involving key stakeholders (including government, communities, and involved or at-risk populations) in both increasing awareness and undertaking prevention strategies.
Key messages
• Rates of congenital syphilis have risen in Canada after outbreaks of infectious syphilis in some locales.
• Routine screening for syphilis remains the standard of care for all pregnant women; those at high risk for syphilis should be rescreened later in pregnancy or at delivery.
• Pregnant women with infectious syphilis should be treated with benzathine penicillin G at a dosage appropriate for the mother's stage of infection; sexual partners should be located and also treated.
• Pregnant women with infectious syphilis, particularly after 20 weeks of gestation, should be managed in conjunction with a maternal–fetal specialist and with ultrasound evaluations.
• Infants born to mothers who have infectious syphilis should be assessed by or in conjunction with a specialist pediatrician; those who require treatment should be treated with crystalline penicillin G administered intravenously, and intense clinical and serologic follow-up should be provided.
Footnotes
-
Consent to publish non-nominal information about the cases in this article was provided by Dr. K. Grimsrud, Acting Chief Medical Officer of Health, Alberta Health and Wellness.
In spite of treatment the most prolonged, the most strictly followed, and the best suited to the nature of the symptoms, it is never perfectly certain that they will not return. Consequently, we can never have the positive assurance that the germ of syphilis is altogether extinct, that it will not reveal its survival by the birth of a contaminated child. — Paul Diday, A Treatise on Syphilis in Newborn Children and Infants at the Breast. London; 1859.
This article has been peer reviewed.
Acknowledgements: We are indebted to the staff of the Capital Health STD Centre, Alberta Health and Wellness STD Services and Provincial Laboratory for Public Health for the provision of data and outstanding clinical care.
Competing interests: None declared.