Evidence Summary

Syphilis Infection in Pregnant Women: Screening

September 04, 2018

Recommendations made by the USPSTF are independent of the U.S. government. They should not be construed as an official position of the Agency for Healthcare Research and Quality or the U.S. Department of Health and Human Services.

By Jennifer S. Lin, MD; Michelle L. Eder, PhD; and Sarah I. Bean, MPH

The information in this article is intended to help clinicians, employers, policymakers, and others make informed decisions about the provision of health care services. This article is intended as a reference and not as a substitute for clinical judgment.

This article may be used, in whole or in part, as the basis for the development of clinical practice guidelines and other quality enhancement tools, or as a basis for reimbursement and coverage policies. AHRQ or U.S. Department of Health and Human Services endorsement of such derivative products may not be stated or implied.

This article was published in JAMA on September 4, 2018.

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Importance: The incidence of syphilis and congenital syphilis in the United States has increased after reaching historic lows in the early 2000s.

Objective: To systematically review literature on the effectiveness and harms of screening for syphilis in pregnancy and the harms of penicillin treatment in pregnancy to inform the US Preventive Services Task Force.

Data Sources: MEDLINE, PubMed, and the Cochrane Central Register of Controlled Trials for relevant English-language literature, published from January 1, 2008, to June 2, 2017. Ongoing surveillance was conducted through November 22, 2017.

Study Selection: Studies conducted in countries categorized as “high” or “very high” on the Human Development Index that explicitly addressed 1 of 3 a priori–defined key questions.

Data Extraction and Synthesis: Independent critical appraisal and data abstraction by 2 reviewers. Data from included studies were narratively synthesized without pooling data.

Main Outcomes and Measures: Incidence of congenital syphilis; any harms of screening or penicillin treatment in pregnancy.

Results: Seven studies in 8 publications were included. One observational study evaluated the implementation of syphilis screening in pregnancy in 2,441,237 women in China. From 2002 to 2012, screening for syphilis in all pregnant women increased from 89.8% to 97.2%, and the incidence of congenital syphilis decreased from 109.3 to 9.4 cases per 100,000 live births. Five studies (n = 21,795) evaluated the false-positive findings of treponemal tests and 1 study (n = 318) evaluated the false-negative findings of nontreponemal tests. These studies found that false-positives with treponemal-specific enzyme or chemiluminescent immunoassays were common (46.5%-88.2%), therefore warranting reflexive (automatic confirmatory) testing for all positive test findings. One study (n = 318) found no false-negatives with treponemal tests, and 1 study (n = 139) demonstrated the prozone phenomenon (false-negative response from high antibody titer) with rapid plasma reagin screening using undiluted samples (2.9%). No studies were identified for harms of penicillin in pregnancy.

Conclusions and Relevance: Screening for syphilis infection in pregnant women is associated with reduced incidence of congenital syphilis, and available evidence supports the need for reflexive testing for positive test results.

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In the United States, the rate of reported congenital syphilis was 15.7 cases per 100,000 live births in 2016, the highest rate reported since 2001.1,2 Congenital syphilis is an infectious disease caused by the vertical transmission of Treponema pallidum; thus, prevention and detection of congenital syphilis depend on the identification of syphilis in pregnant women. Two screening protocols are commonly used: the traditional screening algorithm (ie, nontreponemal testing with reflex to treponemal testing) and the reverse sequence screening algorithm (ie, treponemal testing with reflex to nontreponemal testing) (Figure 1).3,4 Untreated syphilis in pregnancy carries significant risk for stillbirth or fetal loss, premature birth, low birth weight, congenital syphilis, and neonatal death.5,6 Parenteral benzathine penicillin G is the only recommended antibiotic for preventing maternal transmission of syphilis to the fetus and treating fetal syphilis infection.7 This evidence review was completed to inform the US Preventive Services Task Force (USPSTF) in the update to its 2009 “A” recommendation to screen all pregnant women for syphilis.8,9

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Scope of Review

Because this topic represents well-established, evidence-based standards of practice, the USPSTF commissioned a targeted review using an updating process known as “reaffirmation,” which aims to identify “new and substantial evidence sufficient enough to change the prior recommendation.”10,11 As such, only the interval evidence for targeted key questions from the previous systematic review is included. After members of the USPSTF were consulted, an analytic framework and 3 key questions (KQs) were developed to guide the evidence update (Figure 2). Detailed methods and results, including evidence to address the effect of repeat testing for syphilis in the third trimester, at delivery, or both, are available in the full evidence report at https://www.uspreventiveservicestaskforce.org/uspstf/recommendation/syphilis-infection-in-pregnancy-screening.

Data Sources and Searches

MEDLINE, PubMed (publisher-supplied references only), and the Cochrane Central Register of Controlled Trials were searched from January 1, 2008, to June 2, 2017. In addition to these searches, reference lists of existing reviews and primary studies were scanned. Searches were limited to articles published in English. Active surveillance via article alerts and targeted searches of high–impact factor journals to identify major studies published in the interim was conducted through November 22, 2017.

Study Selection

Two reviewers independently reviewed 453 unique citations and 34 full-text articles against a priori inclusion criteria (Figure 3). For all KQs, studies conducted in countries categorized as “high” or “very high” on the Human Development Index were included. For evidence on the benefits of screening for syphilis in pregnancy (KQ1), randomized or nonrandomized controlled intervention studies and large before-after or ecologic studies reporting the association of implementing a screening program with the incidence of congenital syphilis and other adverse outcomes in pregnant women with syphilis were included. For evidence on the harms of screening (KQ2), studies in pregnant women that reported psychosocial harms, stigma, and screening test inaccuracy (ie, false-positive or false-negative results) were included. For KQ1 and KQ2, studies of screening for syphilis in asymptomatic pregnant women using either traditional or reverse sequence algorithms were selected. Studies of screening tests not currently used in US primary care settings and studies in women living with HIV were excluded. For evidence on the harms of treatment (KQ3), studies of penicillin treatment for syphilis in pregnant women that reported any maternal or neonatal harms were included.

Data Extraction and Quality Assessment

Independent critical appraisal of included trials was conducted by 2 reviewers using predefined criteria, with disagreements resolved by discussion. Each study was rated as good, fair, or poor quality. A good-quality study met all quality criteria. A fair-quality study failed to meet at least 1 criterion but had no known issue that would invalidate its results. Studies were rated as poor quality if they had major risk of bias. No studies were excluded for poor quality. Important study and participant characteristics and outcomes were abstracted and subsequently checked by a second reviewer for accuracy and completeness

Data Synthesis and Analysis

Data from 7 studies (reported in 8 publications) were summarized in a narrative format, with an accompanying summary table for KQ2.

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Benefits of Screening

Key Question 1. Does screening for syphilis in pregnant women reduce the incidence of congenital syphilis in newborns?

One fair-quality observational study, which used both historical and geographic comparators, was designed to evaluate the implementation of free syphilis screening (with follow-up and treatment) among all pregnant women living in the region of Shenzhen, China.12 This study was included in the last evidence update to support the 2009 recommendation statement; however, results from longer-term follow-up have since been published. All pregnant women from January 2002 to December 2012 in 90 hospitals in Shenzhen (n = 2,441,237) were offered syphilis and HIV screening. A nontreponemal test was used to screen for syphilis, with reflex to treponemal testing if the test result was positive. Women testing positive for syphilis by serology were given follow-up visits and treatment (including health education), partner notification, and the opportunity to terminate their pregnancy. Women who chose to continue their pregnancies were treated with 3 injections of penicillin G (2.4 million units intramuscularly) at weekly intervals.

From 2002 to 2012, 8455 of the 2,441,237 pregnant women screened tested positive for syphilis.12 The timing of screening, treatment, or both (eg, if screening, treatment, or both occurred earlier in pregnancy in later years) was not reported. From 2002 to 2012, screening for syphilis in all pregnant women increased from 89.8% to 97.2%, and the incidence of congenital syphilis decreased from 109.3 to 9.4 cases per 100,000 live births. During this same period, in pregnant women infected with syphilis, the incidence of all adverse outcomes declined from 42.7% to 19.2%; incidence of congenital syphilis declined from 11.7% to 3.2%; and incidence of stillbirth or fetal loss declined from 19.0% to 3.3%. Although this study does not include an historical comparator (ie, a time point before implementation of the screening program) because the screening program was initiated in 2001 and screening commenced in 2002, the authors also report the incidence of congenital syphilis in Shenzhen compared with the national incidence. From 2002 to 2012, the incidence of congenital syphilis in China increased from 5.9 to 97.4 cases per 100,000 live births, while incidence of congenital syphilis specifically in Shenzhen decreased from 109.3 to 9.4 cases per 100,000 live births. No P values are reported for any of these comparisons or trends of outcomes. Despite methodological limitations (with both the historical and geographic comparisons) and concerns about applicability to US practice (timing of screening; treatment options, including termination of pregnancy and use of erythromycin for women with penicillin allergies), this study provides observational evidence that screening for, coupled with treatment of, syphilis in pregnancy is associated with a decrease in incidence of congenital syphilis.

Harms of Screening

Key Question 2. What are the harms of screening for syphilis in pregnant women?

Five new studies (n = 21,795) that reported on false-positive results of treponemal tests were identified,13-17 1 of which also reported on false-negative results,17 along with 1 new study (n = 318) that reported on false-negative results of nontreponemal testing (Table 1).18 No studies were found that addressed the diagnostic inaccuracy of the entire screening algorithm or other potential harms of screening for syphilis in pregnant women. Four large, fair-quality retrospective studies evaluated the proportion of false-positive results using treponemal-specific enzyme immunoassays (EIAs) or chemiluminescent immunoassays (CIAs) in screening pregnant women for syphilis.13-16 These studies found that false-positives with EIA or CIA were common (46.5% to 88.2%), therefore warranting reflexive (automatic confirmatory) testing for all positive CIA or EIA test results. None of the studies reported confidence intervals for false-positives.

One fair-quality prospective study evaluated the diagnostic accuracy of CIA and the T pallidum particle agglutination assay (TPPA) in 318 pregnant women.17 This study had only 1 positive result from CIA testing and 2 positive results from TPPA testing and therefore could not provide robust estimates of false-positives. This study found no false-negatives for any test.

One fair-quality retrospective study (n = 139) evaluated the prozone phenomenon using rapid plasma reagin (RPR) testing.18 The prozone phenomenon occurs when undiluted serum containing a high titer of nonspecific antibody (as may occur in secondary syphilis) produces a false-negative result attributable to a large quantity of antibodies occupying all the antigen sites (preventing flocculation).3 This study repeated RPR testing in discordant samples (RPR-negative/TPPA-positive) using diluted serum and found that 2.9% of discordant samples had a false-negative RPR result attributable to the prozone phenomenon.

Harms of Treatment

Key Question 3. What are the harms of treatment of syphilis with penicillin during pregnancy to pregnant women or newborns?

No studies directly examining the harms of penicillin in pregnancy and meeting the inclusion criteria were identified. In particular, no studies were found that addressed the risk of the Jarisch-Herxheimer reaction or serious adverse events in women with a history of penicillin allergy.

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The findings of this brief evidence review support the understanding that screening for syphilis early in pregnancy reduces congenital syphilis and also support the need for reflexive testing to investigate initial positive EIA/CIA test results in reverse sequence screening (Table 2). Screening for syphilis at the first prenatal visit to prevent congenital syphilis is standard of care and legally mandated in most US states.19 Observational evidence not included in this review supports the effectiveness of identification and treatment of syphilis in pregnancy to avoid adverse outcomes of pregnancy and specifically supports identification and treatment as early as possible in pregnancy (as opposed to in the third trimester or at delivery).5,12,20

This update includes longer-term follow-up from an observational study evaluating the implementation of syphilis screening in more than 2 million pregnant women in Shenzhen, China, demonstrating an approximate 11-fold decrease in the incidence of congenital syphilis over 10 years. Screening for syphilis using treponemal and nontreponemal tests in combination is feasible for mass screening and provides a presumptive laboratory diagnosis of syphilis with high accuracy and reliability. Because of the false-positive test results with initial treponemal testing (ie, CIA or EIA) and a negative RPR and TPPA result in low-risk patients or low-prevalence populations, clinician education on the reverse sequencing algorithm and interpretation and limitations of syphilis serologic test results in general is critical to avoid overdiagnosis or underdiagnosis and treatment errors. Evidence from this review confirms concern for false-positives with treponemal-specific screening tests in low-risk pregnant females when the RPR result is negative and the prozone phenomenon has been ruled out, supporting the rationale for treponemal reflexive testing. Penicillin G is generally accepted to be effective and safe for use in pregnancy. Observational data support the effectiveness of benzathine penicillin G in preventing congenital syphilis when the mother is treated early in pregnancy, and serious harms are uncommon5,6; however, good-quality evidence in pregnant women is lacking.21 The Jarisch-Herxheimer reaction, which can induce early labor or cause fetal distress in pregnant women, albeit rarely, is more common in primary and secondary syphilis during pregnancy and cannot be mitigated with a different choice of antibiotic.

Limitations

This review was intended to support the USPSTF reaffirmation process and thus includes only the interval evidence accrued since the last recommendation in 2009. The review was scoped to identify evidence that could result in a change in this recommendation and therefore has some notable exclusions. First, it did not include studies addressing the effectiveness of screening or early prenatal care in low- or middle-income countries, because these studies were less applicable to prenatal care in the United States. Second, the review did not address the comparative screening accuracy of traditional vs reverse sequence algorithm testing; however, to our knowledge, no studies have compared these 2 testing algorithms in prenatal care. Third, the benefit of penicillin G for the treatment of syphilis is well established, so new evidence for this question was not included. Fourth, because the review was primarily focused on screening, it did not address the efficacy of alternative antibiotic treatments (eg, ceftriaxone) in pregnant women (with or without penicillin allergies).

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Screening for syphilis infection in pregnant women is associated with reduced incidence of congenital syphilis, and available evidence supports the need for reflexive testing for positive test results.

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Source: This article was first published in the Journal of the American Medical Association on September 4, 2018 (JAMA. 2018;320(9):918-925).

Conflict of Interest Disclosures: All authors have completed and submitted the ICMJE Form for Disclosure of Potential Conflicts of Interest and none were reported.

Funding/Support: This research was funded under contract HHSA290201200015I, Task Order 5, from the Agency for Healthcare Research and Quality (AHRQ), US Department of Health and Human Services, under a contract to support the USPSTF.

Role of the Funder/Sponsor: Investigators worked with USPSTF members and AHRQ staff to develop the scope, analytic framework, and key questions for this review. AHRQ had no role in study selection, quality assessment, or synthesis. AHRQ staff provided project oversight, reviewed the report to ensure that the analysis met methodological standards, and distributed the draft for peer review. Otherwise, AHRQ had no role in the conduct of the study; collection, management, analysis, and interpretation of the data; and preparation, review, or approval of the manuscript findings. The opinions expressed in this document are those of the authors and do not reflect the official position of AHRQ or the US Department of Health and Human Services.

Additional Information: A draft version of this evidence report underwent external peer review from 5 content experts (Robert Phillips Heine, MD, Duke University School of Medicine; Jeanne S. Sheffield, MD, Johns Hopkins School of Medicine; and 3 individuals from the US Centers for Disease Control and Prevention). Comments from reviewers were presented to the USPSTF during its deliberation of the evidence and were considered in preparing the final evidence review.

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1. Bowen V, Su J, Torrone E, Kidd S, Weinstock H. Increase in incidence of congenital syphilis—United States, 2012-2014. MMWR Morb Mortal Wkly Rep. 2015;64(44):1241-1245. doi:10.15585/mmwr.mm6444a3
2. Centers for Disease Control and Prevention. Sexually Transmitted Disease Surveillance 2016. Atlanta, GA: U.S. Dept. of Health and Human Services; 2017.
3. Morshed MG, Singh AE. Recent trends in the serologic diagnosis of syphilis. Clin Vaccine Immunol. 2015;22(2):137-147. doi:10.1128/CVI.00681-14
4. Centers for Disease Control and Prevention (CDC). Discordant results from reverse sequence syphilis screening—five laboratories, United States, 2006-2010. MMWR Morb Mortal Wkly Rep. 2011;60(5):133-137.
5. Gomez GB, Kamb ML, Newman LM, Mark J, Broutet N, Hawkes SJ. Untreated maternal syphilis and adverse outcomes of pregnancy: a systematic review and meta-analysis. Bull World Health Organ. 2013;91(3):217-226. doi:10.2471/BLT.12.107623
6. Qin J, Yang T, Xiao S, Tan H, Feng T, Fu H. Reported estimates of adverse pregnancy outcomes among women with and without syphilis: a systematic review and meta-analysis. PLoS One. 2014;9(7):e102203. doi:10.1371/journal.pone.0102203
7. Workowski KA, Bolan GA; Centers for Disease Control and Prevention. Sexually transmitted diseases treatment guidelines, 2015. MMWR Recomm Rep. 2015;64(RR-03):1-137.
8. U.S. Preventive Services Task Force. Screening for syphilis infection in pregnancy: U.S. Preventive Services Task Force reaffirmation recommendation statement. Ann Intern Med. 2009;150(10):705-709. doi:10.7326/0003-4819-150-10-200905190-00008
9. Wolff T, Shelton E, Sessions C, Miller T. Screening for syphilis infection in pregnant women: evidence for the U.S. Preventive Services Task Force reaffirmation recommendation statement. Ann Intern Med. 2009;150(10):710-716. doi:10.7326/0003-4819-150-10-200905190-00009
10. Patnode CD, Eder ML,Walsh ES, Viswanathan M, Lin JS. The use of rapid review methods for the U.S. Preventive Services Task Force. Am J Prev Med. 2018;54(1S1):S19-S25. doi:10.1016/j.amepre.2017.07.024
11. U.S. Preventive Services Task Force. U.S. Preventive Services Task Force Procedure Manual. Rockville, MD: Agency for Healthcare Research and Quality; 2015.
12. Qin JB, Feng TJ, Yang TB, et al. Synthesized prevention and control of one decade for mother-to-child transmission of syphilis and determinants associated with congenital syphilis and adverse pregnancy outcomes in Shenzhen, South China. Eur J Clin Microbiol Infect Dis. 2014;33(12):2183-2198. doi:10.1007/s10096-014-2186-8
13. Boonchaoy A, Wongchampa P, Hirankarn N, Chaithongwongwatthana S. Performance of chemiluminescent microparticle immunoassay in screening for syphilis in pregnant women from low-prevalence, resource-limited setting. J Med Assoc Thai. 2016;99(2):119-124.
14. Wang KD, Xu DJ, Su JR. Preferable procedure for the screening of syphilis in clinical laboratories in China. Infect Dis (Lond). 2016;48(1):26-31. doi:10.3109/23744235.2015.1044465
15. Mmeje O, Chow JM, Davidson L, Shieh J, Schapiro JM, Park IU. Discordant syphilis immunoassays in pregnancy: perinatal outcomes and implications for clinical management. Clin Infect Dis. 2015;61(7):1049-1053. doi:10.1093/cid/civ445
16. Henrich TJ, Yawetz S. Impact of age, gender, and pregnancy on syphilis screening using the Captia Syphilis-G assay. Sex Transm Dis. 2011;38(12):1126-1130. doi:10.1097/OLQ.0b013e31822e60e1
17. Wellinghausen N, Dietenberger H. Evaluation of two automated chemiluminescence immunoassays, the LIAISON Treponema Screen and the ARCHITECT Syphilis TP, and the Treponema pallidum particle agglutination test for laboratory diagnosis of syphilis. Clin Chem Lab Med. 2011;49(8):1375-1377. doi:10.1515/CCLM.2011.643
18. Liu LL, Lin LR, Tong ML, et al. Incidence and risk factors for the prozone phenomenon in serologic testing for syphilis in a large cohort. Clin Infect Dis. 2014;59(3):384-389. doi:10.1093/cid/ciu325
19. Warren HP, Cramer R, Kidd S, Leichliter J. State prenatal syphilis screening policies in the United States, 2016 [published online July 17, 2018]. Matern Child Health J. doi:10.1007/s10995-018-2592-0
20. Hawkes SJ, Gomez GB, Broutet N. Early antenatal care: does it make a difference to outcomes of pregnancy associated with syphilis? a systematic review and meta-analysis. PLoS One. 2013;8(2):e56713. doi:10.1371/journal.pone.0056713
21. Galvao TF, Silva MT, Serruya SJ, et al. Safety of benzathine penicillin for preventing congenital syphilis: a systematic review. PLoS One. 2013;8(2):e56463. doi:10.1371/journal.pone.0056463

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Figure 1 is a flow diagram adapted from the CDC that depicts the two serologic screening algorithms for syphilis. The traditional screening algorithm uses an initial nontreponemal test with reflex to treponemal testing for initial test positivity. The reverse sequence screening algorithm uses an initial treponemal specific test with reflex to nontreponemal testing for initial test positivity. In the reverse sequence screening algorithm, discordant testing (i.e., initial treponemal test positive, nontreponemal test negative) is confirmed using a second treponemal specific test.

CIA indicates chemiluminescent immunoassay; EIA, enzyme immunoassay; RPR, rapid plasma reagin; TPPA, Treponema pallidum particle agglutination.

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Figure 2 is the analytic framework that depicts the three Key Questions addressed in the systematic review. The figure illustrates the overarching question addressing the effectiveness of screening for syphilis in pregnant women (KQ1) and its relationship to the two additional questions addressing the harms of screening for syphilis in pregnant women (KQ2) and the harms of treatment of syphilis with penicillin during pregnancy (KQ3).

Evidence reviews for the US Preventive Services Task Force (USPSTF) use an analytic framework to visually display the key questions that the review will address to allow the USPSTF to evaluate the effectiveness and safety of a preventive service. The questions are depicted by linkages that relate to interventions and outcomes. Further details are available from the USPSTF procedure manual.11

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Source Patient Selection
(No. of
Pregnant Women
Screened)
Study Design
(Years)
Test Evaluated Cutoff Testing Strategy No. of Positive or Negative Results/Total No. of Tests (%) No. of False-Positive or False-Negative
Results/Total No. of Positive or Negative Results (%)
Quality
Reported Harm: False-Positive Results
Treponemal-specific
CIA
Boonchaoy et al,13 2016
(Thailand)
Pregnant women only
(11,640)
Retrospective (2011-2013) ARCHITECTa S/CO value ≥1.00 Reflex testing with RPR and TPPA 65/11,640 (0.56) 35/65 (53.8) Fair
Wang et al,14 2016
(China)
General population, including pregnant women
(9600)
Retrospective
(2013)
ARCHITECTa S/CO value >1.00 Reflex testing with TPPA; immunoblot used for confirmation of discordant samples 34/9600 (0.35) 30/34 (88.2) Fair
Mmeje et al,15 2015
(United States)
Pregnant women only (NRb) Retrospective
(2007-2010)
LIAISONc NR Reflex testing with RPR and TPPA NR 156/194d (80.4) Fair
Wellinghausen and Dietenberger,17 2011
(Gemany)
General population, including pregnant women
(318)
Prospective
(2010)
ARCHITECTa Index ≥1.0 Reflex testing with FTA-ABS; immunoblot used for confirmation of discordant samples 0/318 (0) NA Fair
LIAISONc Index ≥0.9 Reflex testing with FTA-ABS; immunoblot used for confirmation of discordant samples 1/318 (0.31) 0/1 (0)
Treponemal-specific
EIA
Henrich and Yawetz,16 2011
(United States)
General population, including pregnant women
(NRe)
Retrospective
(2004-2007)
Syphilis-Gf NR Reflex testing with RPR and TPPA NR 20/43g (46.5) Fair
TPPA
Wellinghausen and Dietenberger,17 2011
(Germany)
General population, including pregnant women
(318)
Prospective
(2010)
TPPA Titer ≥1:80 Reflex testing with FTA-ABS; recombinant IgG and IgM immunoblot used for confirmation of discordant samples 2/318 (0.63) 1/2 (50) Fair
Reported Harm: False-Negative Results
RPR
Liu et al,18 2014
(China)
General population, including pregnant women
(NR)
Retrospective
(2010-2013)
RPR
TPPA
RPR: Reactive at dilution of 1:1
TPPA: Titer ≥1:80
RPR test repeated for RPR−, TPPA+ samples using serum diluted to 1:32

Reflex testing of TPPA+ samples with CIA
NR 4/139 (2.9) (prozone phenomenon) Fair
Treponemal-specific
CIA
Wellinghausen and Dietenberger,17 2011
(Gemany)
General population, including pregnant women
(318)
Prospective
(2010)
ARCHITECTa Index ≥1.0 Reflex testing with FTA-ABS; immunoblot used for confirmation of discordant samples 0/318 (0) 0/317 (0) Fair
LIAISONc Index ≥0.9 Reflex testing with FTA-ABS; immunoblot used for confirmation of discordant samples 1/318 (0.31) 0/317 (0)
TPPA
Wellinghausen and Dietenberger,17 2011
(Germany)
General population, including pregnant women
(318)
Prospective
(2010)
TPPA Titer ≥1:80 Reflex testing with FTA-ABS; recombinant IgG and IgM immunoblot used for confirmation of discordant samples 2/318 (0.63) 0/316 (0) Fair

Abbreviations: CIA, chemiluminescent immunoassay; EIA, enzyme immunoassay; FTA-ABS, fluorescent treponemal antibody absorption test; NA, not applicable; NR, not reported; RPR, rapid plasma reagin; S/CO, ratio of optical density value of samples to cutoff; TPPA, Treponema pallidum particle agglutination.
a The ARCHITECT Syphilis TP Assay (Abbott) is a chemiluminescent microparticle immunoassay for the qualitative detection of antibodies (IgG and IgM) directed against Treponema pallidum in human serum and plasma.
b All pregnant women tested with reverse sequence algorithm at Kaiser Permanente Northern California.
c The LIAISON Treponema Assay (DiaSorin) uses CIA technology for the qualitative determination of total antibodies directed against T pallidum in human serum.
d One hundred ninety-four women with CIA-positive, RPR-negative serology results.
e All pregnant women screened with IgG EIA at first prenatal visit.
Syphilis (T pallidum)-G (CAPTIA) is an EIA for the qualitative detection of IgG antibodies to T pallidum in serum specimens.
g Forty-three pregnant women with positive EIA results.

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Rationale and Foundational Evidence New Evidence Findings Limitations of New Evidence Consistency of New Evidence With Foundational
Evidence and Current Understanding
Benefits
Screening: Observational studies demonstrate the association of lower adverse outcomes of pregnancy in women with syphilis infection treated in pregnancy vs those not treated

Treatment: Parenteral penicillin G is highly effective in treating maternal syphilis and preventing congenital syphilis
Screening: One observational study evaluating the implementation of screening for syphilis in >2 million pregnant women in Shenzhen, China, demonstrated an 11-fold decrease in congenital syphilis over 10 y12

Treatment: Not readdressed
Included observational study has significant methodologic limitations (ie, with the use of historical and geographic comparators), as well as significant concerns around external validity of findings (eg, national data from China suggest a syphilis epidemic)

The magnitude of benefit in US practice will depend on underlying rates of syphilis in local practice settings
Included observational study is consistent with the understanding that universal screening for syphilis early in pregnancy can prevent congenital syphilis
Harms
Screening: No severe adverse outcomes, as screening only requires blood testing (widely available) and these tests (treponemal and nontreponemal) in combination detect syphilis with high accuracy and reliability

Treatment: Parenteral penicillin G is generally accepted as safe; however, evidence is limited in pregnant women
Screening: Five studies demonstrated that false-positive results with CIA or EIA in pregnancy are common.13-17 One study demonstrated that undiluted
serum with high titers of nontreponemal antibodies can result in false-negative RPR testing results18

Treatment: No new studies examining harms of treatment in pregnant women were identified
Included diagnostic accuracy studies only report on the test inaccuracy of initial treponemal or nontreponemal test and not the inaccuracy of the entire testing sequence

Different CIA and EIA tests may have varying test (in)accuracy
Included studies confirm that CIA and EIA should be used in combination with reflexive testing to screen for syphilis because false-positive results are common in pregnancy (as well as cannot distinguish between old and current infection)

Abbreviations: CIA, chemiluminescent immunoassay; EIA, enzyme immunoassay; RPR, rapid plasma reagin.

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