Laborator y s t ud y Seropersistent VDRL test reactivity in older age groups 
Evulence oj seropersi.stent VDRL test 
reactivity in an e/Llerly 
Treponema pall"idum-
infected popuuition 
V. Muic, M. Ljubicic, I. Vodopija and V. Mayer 
ABSTRACT 
Background. Using the VDRL test as the only one, ar the first in a series of tests, leads to a diagnostic 
miss in the serological detection of latent and late syphilis, especially among older age group. We 
compared the age of 518 Treponema pa/lidum-infected individuals with their VDRL test results. This was 
aimed at determining the proportion of VDRL reactors who were suspected of having a persistently 
active syphilitic process. 
Methods. Our retrospective analysis of archival data on subjects' age and VDRL serotest outcomes far 
the 518 Treponema pa//idum-infected (who were reactors in the TPHA reference test) covered the period 
197 4-98. They were selected from a nonvenerological population routinely tested at a public health 
laboratory. 
Results. Data analysis revealed the subjects' high mean age (53.13 years in VDRL reactors and 51.87 
years in nonreactors), and an unexpectedly high proportion of VDRL reactors (49%) among those tested. 
Conclusion. It may be presumed based on the 49% persistence of VDRL reactivity coupled with the 
subjects' high mean age (53.15 years), which is appropriate to latent and late syphilis, that most subjects 
(70%) had either been untreated ar insufficiently treated. This view is based on the Bayes' theorem, 
which takes account of the generally accepted percentage of VDRL reactivity far latent and late syphilis. 
Introduction 
In the course of proficiency testing program for the 
serological diagnosis of syphilis in Croatian laboratories 
from 1993 to 1995 we notecl occasional differences in 
inclications for the VDRL serological test (1,2). The first 
stage of that survey checked how proficient routine 
laboratories were in detecting the infected (3), then the 
Acta Dermatoven APA Vol 9, 2000, No 1 
size of cliagnostic miss in cletecting the· latent and late 
(ancl possibly active) syphilis. The then small sample 
uncovered a disproportion between the age of sero-
logically stabilized patients (VDRL nonreactors, but 
TPHA reactors) ancl that of potentially active (VDRL and 
TPHA reactors); also, we noticed the high proportion 
23 
Seropersistent VDRL test reactivity in older age groups 
ofthe latter among the infected. Analysis only included 
the results of a one-tum (actually the last) serological 
testing. Beside the demographic data there were no 
clinical or epidemiological data available on any of the 
subjects tested. Analyzing the above mentioned 
phenomena the present paper attempts to establish the 
causes of the unexpected test reactivity of some po-
pulation subgroups, as well as obtain more information 
about the disease and the affected population. 
Materials and methods 
Tested population. A retrospective analysis of archi-
val data on 518 serologically tested persons, 275 (53%) 
males and 243 ( 47%) females, covered a 22-year period 
0976-98). They unde1went two parallel tests for syphilis 
each: the nontreponemal VDRL test and the treponemal 
TPHA test. 
A public health population was tested whose sera 
are usually studied in puhlic health laboratories: 
non-venereal inpatients, chronic psychiatric asylum 
patients, patients from psychiatric wards and homes, 
persons from conscription centers, prisons etc.; persons 
undergoing pre-employment examinations, persons 
seeking medica! certificates or international health 
documents, pregnant women, etc. Statistical analysis 
covered the items of age, year of testing (1976 through 
1998), sex and the result of parallel testing by the VDRL 
and TPHA tests. 
Tests. Both the VDRL and the TPHA test, which came 
Laborator y study 
from the Croatian Institute ofimmunology, respectively 
BAG GmbH, Germany (TPHA) were done in the stan-
dard way ( 4). Qualitative expression of the results en-
abled the use of literature data from nosological sen-
sitivity and specificity tables in function of the stage of 
syphilitic process and subject status as treated or 
untreated. Throughout the period studied (1974-98), the 
problem sera were subject to proficiency testing 
performed by N.A. Johnston of the V.D. Reference 
Laborat01y P.H.L.S., The London Hospital, London, E.1, 
Great Britain. 
Statistical procedures. In addition to the standard 
statistical methods an own statistical procedure was used 
which is based on the Bayes' theorem (5). In the absence 
of clinical data this allowed us to assess the proportion 
of untreated among the infected. 
Results 
For greater clarity the tested population was divided 
into 3 groups by tirne periods, thus permitting a statistical 
evaluation to detect eventual differences. Table 1. 
During the 1976-1979 period 77 patients' sera were 
tested: 59 were VDRL+ TPHA+; the arithmetical mean 
value oftheir ages was 50.45 years. In the same period 
18 sera were VDRL- TPHA +, their ages giving the mean 
value of 52.59 years. Figure l. 
There were 130 patients' sera tested during the 1990-
98 period: 52 were VDRL+ TPHA+, their mean ari-
Table 1. The number ofpersons tested by test periodfrom 1976 to 1998, and the arithmetic mean ageforpersons 
with d{ff'ering results qlcombined parallel testing: VDRL+ TPHA+ and VDRL-TPHA+. 
1976-1979 77 1 50.45 52.59 
1980-1989 311 2 52.54 53.27 
1990-1998 130 3 58.56" 49.06 
Weighted arithmetic mean age 53.13b 51.87c 
(N=254, N=264 and N=518) 52.69d 
TOTAL 518 
"The dividing of this group by sex uncovered a temale VDRL and TPHA reactive group with high arithmetic 
mean age of 63.94 years, as well as its highly statistically significant (p<0.008) age difference in relation to the 
all-subject (518) arithmetic mean age of 52.69 years. 
1, The data relate to N=254. 
c The data relate to N=264. 
c1 The dara relate to N=518. 
24 Acta Dermatoven APA Vol 9, 2000, No 1 
Laborator y study 
s o 
a, · 
-.;s 
:::J 
ti) 
o~ 
o z ·· 
24..-------~-------------------, 
22.. . 
20· 
16. 
14 
12" 
:t:O: 
-e 
s: 
"4" 
2 
G 
o- ro- 20 so- nr so-· 90 
rcr- year age groups 
Figure 1. The number of subjects with VDRL+ TPHA+ test results 
(N=59; arithmetic mean age = 50.45 yr.) and VDRL- TPHA+ results 
(N=18; arithmetic mean age = 52.59 yr.) by 10-year age groups in 
the 1976-79 period. 
thmetical age was 58.56 years, while 78 were VDRL-
TPHA + with a mean arithmetical age of 49.06 years. 
Figure 2. 
Inserting our data on VDRL positive tests amounting 
to 49% (VDRL sensitivity) of all the infected (TPHA 
positives) into the Bayes theorem-based formu la (5), 
Figure 2. The number of subjects testing VDRL+ TPHA+ (N=52, 
arithmetic mean age = 58.56) and VDRL- TPHA+ 
(N=78, arithmetic mean age = 49.06) by 10-year age groups in the 
period 1990-98. 
24..---------------------------, 
o- 1 o- ~ 30 40 - 5G- 60- 70 -89- 9G-- 100 
1 O - year age groups 
Acta Dermatoven APA Vol 9, 2000, No 1 
Seropersistent VDRL test reactivity in older age groups 
together with VDRL sensitivity data for treated (1 %) and 
untreated (70%) yielded a proportion of 0.7, an 
indication that 70% of our infected subjects had probably 
not been treated. Inserting in the same formula for the 
sensitivity of the treated a value of 10%, this would still 
give a high value of 65% for the untreated. 
Discussion 
The presence for 22 years in public health labora-
tory's records of a high percentage ( 49%) ofVDRL reac-
tors with an average age of over 50 years could be consi-
dered unexpected. Actually, it is assumed that for sero-
positive cases aged 50 years sufficient tirne has elapsed 
since their infection and treatment ( which most probably 
happened in their 20s) for VDRL findings to turn 
negative. However, in contradiction to the available lite-
rature stating that persistent serological reactivity on the 
VDRL test is a rare phenomenon (6), through subse-
quent decades (probably during some 30 years) only 
half our subjects tested negative on the VDRL. The 
literature VDRL reactor values for treated late latent 
syphilis and treated late manifest syphilis are 1 % only 
(7). Though higher values may have been reported, they 
were unaccompanied by a specification as to the interval 
lapsed between the times of treatment and testing (6,8) . 
Moreover, not even untreated latent syphilis or late sy-
philis exceed the VDRL reactivity of 70% (30% of the 
diseased spontaneously become negative) (6). Based 
on the above, one could hypothesize that a large portion 
of our subjects had either received no treatment or an 
inadequate one. The successfully treated minority pro-
bably contributed 20% of the negative tests, thus 
rounding up the VDRL nonreactors to about 50%. Never-
theless , it would be more correct to assess the old 
population of the infected with regard to previous treat-
ment, orno treatment, by means of the Bayes' theorem-
based procedure which we used in the No. 3 0997) 
issue of this review, presenting the results of the first 
part of the same study (5). Inserting the 1 % reactivity to 
the VDRL reported in the literature for the treated (7), 
and the 70% reactivity to the VDRL test for the untreated 
who have latent and late syphilis (6), as well as our figure 
of 50% for theprevalence of the VDRL reactors, yields, 
in terms of proportion, a result of 0.7. In other words, it 
would appear that 70% of our VDRL positive population 
have not been treated. Had we inserted 10% instead of 
the value of 1 % for VDRL test reactors in the treated that 
would still produce as many as 65% untreated! 
An off hypothesis, i.e. , that our patients had acquired 
syphilis not in their 20s but after turning 40, might be 
proffered to explain the high proportion of VDRL reac-
2.5 
Laborator y study 
tors among our infected subjects . If true, it could be 
argued that despite the patients receiving adequate 
treatment, the reactivity on the VDRL test had not dis-
appeared yet. 
Even less probable is the assumption that our pa-
tients had started their treatment only some 10 years 
after developing the infection, i.e., at the stage of late 
latency and late syphilis. Some authors feel that VDRL 
reactivity could stay in as many as half such subjects 
longer than 2 years (6) or "for years" (8). Nevertheless, 
a growing trend in the number of VDRL nonreactors 
among the infected observed over 22 years points to 
the fact that in the past few years the treatment of syphilis 
has become increasingly effective. 
In addition to the unusually large portion of VDRL 
reactors noticed at the first stage of this study (5), also 
recorded was their higher average age. Statistical 
analysis ona bigger sample of 518 infected has shown 
this phenomenon to be significant only in one subgroup 
ofwomen tested between 1990 and 1998 (Table 1). One 
explanation might be the coincidence between their 
tirne of infection and the start of the penicillin era in 
Croatian hospitals. In fact, the abandonment of strongly 
treponemocidal (but toxic for body) arsenobenzolic 
preparations and bismuth salts, coupled with the use of 
the then insufficient penicillin concentrations and length 
of treatment could have contributed to the pheno-
menon. Another extra factor possibly having the same 
effect was the use of benzathine penicillin, which is 
known for low penetration into some tissues and body 
systems (7). To this one should add the known diffi-
culties of detecting syphilis in women with the resulting 
lat er start of treatment. 
A possibly active syphilitic process could account 
for the high-recorded percentage ofVDRL reactors ( 49% 
of the 518 tested) among the infected and for their high 
mean age (53.13 yr.). This might have public health 
CE S 
Seropersistent VDRL test reactivity in older age groups 
repercussions. The above phenomenon warrants fotther 
corroboration and analyses (clinical follow-up and CSF 
evaluation). It also impresses on nonvenereologists the 
need to cautiously order and interpret serological tests 
for the demonstration of syphilis (6). This subsumes 
quantifying the VDRL among the infected and the use 
of modem tests to determine the intensity of syphilitic 
process. 
Conclusion 
Analyzing for 22 years (1976-96) the relationship bet-
ween the patient's age and VDRL test results ona large 
sample of 518 T pallidum-infected persons revealed a 
high proportion (49%) of subjects (with a mean age 
above 50 years) potentially affected by an active syphi-
litic process (VDRL reactives). Conspicuous among them 
was a female subgroup statistically significant for its high 
age (64 vs. a general average of 52.7 years) (p<0.008). 
It was probably infected and insufficiently treated in 
the arsenobenzol-penicillin switch period. As well as 
indicating a possible presence of an unrecognized active 
syphilis in elderly age, the results point to the need for 
nonvenereologists to exercise care in ordering and inter-
preting syphilis serotests. 
Acknowledgment 
The authors would like to thank Victoria Pope, PhD, 
Chief Treponemal Pathogenesis and Immunology 
Branch, Division of AIDS, STD and TB Laboratory 
Research National Center for Infectious Diseases, CDC, 
Atlanta, USA for valuable advice helping in the comple-
tion of this work. 
They also thank Vilim Crlenjak, BA, from the Cro-
atian National Institute of Public Health for the trans-
lation. 
l. Anonymous. Serological screening methods far the most relevant microbiological diseases of organ 
and tissue donors. European Health Committee, Council of Europe, 25-27 June 1996, CDSP (96) 21, 
p.5. 
Acta Dermatoven APA Vol 9, 2000, No 1 
2. Muic V, Vodopija I. Serotesting far syphilis, diagnostic proficiency and health care quality surveillance 
(in Croatian). Lijec Vjesn 1996; 118: 184-6. 
3. Muic V, Vodopija I, Ljubicic M, Mayer V, Jankovic V. Interlaboratory differences in VDRL test nosologic 
sensitivity in syphilis serodiagnosis in Croatia from 1993 to 1995. Period biol 1997; 99: 45-8. 
4. Larsen S, Hunter E. Syphilis Diagnosis. In: lsenberg H ( ed). Clinical Microbiological Handbook. 
Washington DC, American Society far Microbiology, Supplement 1, 1994, Section 9.7. 
27 
Seropersistent VDRL test reactivity in older age groups Laborator y study 
AUTHORS' 
ADDRESSES 
28 
5. Muic V, Vodopija I, Ljubicic M, Mayer V. Limitations and consequences of basing late syphilis 
seroassessments on VDRL test. Acta Dermatoven APA 1997; 6: 87-91. 
6. Larsen S. Steiner E, Rudolph A. Laboratory diagnosis and interpretation of tests for syphilis. Ciin 
Microbiol Rev 1995; 8:1-21. 
7. Tramont E. Treponema pallidum (Syphilis). In: Mandeli GI, Benett JE, Dolin R, eds. Mandeli, Douglas 
and Benett's Principles of Infectious Diseases. New York, NY: Churchill Livingstone, 1995: 2117-33. 
8. Lukehart S, Holmes K. Syphilis. In: Isselbacher K (ed) Harrison's Principles oflnternal Medicine. New 
York, McGraw Hill, 1994; 726-37. 
Vladimir Muič MD, PhD, consultant, Croatian National Institute oj Pub lic 
Health, 10000 Zagreb, Rockejellerova 7, Croatia. 
Mate Ljubičič, MD, PhD, assist. projessor and director, Croatian National 
Institute oj Pub lic Health, 10000 Zagreb, Rockejellerova 7, Croatia. 
Ivan Vodopija MD, PhD, projessor and consultant, Zagreb Pub lic Health 
Institute, Mirogojska 16, 10000 Zagreb, Croatia 
Vladimir Mayer, MD, PhD, head, Health C are Planning and Programming 
Dept., Croatian National Institute oj Pub lic Health, 10000 Zagreb, 
Rockejellerova 7, Croatia. 
Acta Dermatoven APA Vol 9, 2000, No 1