HPV-associated
Cancer among HIV Positive Men and Women in the Combination ART Era
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| SUMMARY:
Precancerous
anal cell changes and infection with high-risk human papillomavirus
(HPV) types remain common among men with HIV despite effective
antiretroviral therapy (ART) that suppresses viral load and
restores CD4 cell levels, according to a study presented at
the XVIII International AIDS Conference (AIDS
2010) last month in Vienna. A related study found that
invasive cervical cancer -- also caused by HPV -- was associated
with lower CD4 cell counts among HIV positive women in the
large NA-ACCORD cohort. |
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By
Liz Highleyman
Human papillomavirus
is a common sexually transmitted infection that can cause abnormal cell
changes. Several types cause warts, and "high-risk" types
including HPV-16 and HPV-18 can cause malignant cell growth, or cancer.
While invasive cervical cancer is considered an AIDS-defining illness,
anal cancer is not, even though they have the same cause.
Anal
Cancer in Men
In the first study presented at AIDS 2010, Christopher Piketty and colleagues
from the French Valparaiso Study Group aimed to assess the impact of
combination ART and
immune restoration on HPV-related anal cell abnormalities among men
with HIV.
This longitudinal analysis included 94 HIV positive men who have sex
with men (MSM) seen at 7 academic hospitals in France who started combination
ART for the first time. The median age was about 40 years. Only 4% had
ever had an AIDS diagnosis, but about 20% had a history of other sexually
transmitted infections.
The researchers
tested participants for HPV DNA (genetic material), examined anal cells
using ThinPrep Pap smears, and looked for tissue abnormalities including
squamous intraepithelial lesions (SIL), a precursor of anal cancer.
In addition, CD4 and CD8 T-cell responses to the E6 and E7 proteins
of HPV-16 were measured in a subgroup of participants who had anal HPV-16
infection at study entry.
Samples
were obtained at baseline and at months 12 and 24 after starting ART;
12-month data were reported.
Results
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The
researchers identified 56 cases of invasive cervical cancer following
ART initiation, and matched them with 503 controls. |
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Women
with lower CD4 counts were more likely to develop invasive cervical
cancer during follow-up. |
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At
the time of ART initiation, the mean CD4 count was about 240 cells/mm3
in both case and control groups. |
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4
years prior to starting ART, however, the mean CD4 cell count among
women who developed invasive cervical cancer was about 160 cells/mm3
lower than that of control women, a significant difference. |
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At
1 year after ART initiation, average CD4 count was about 40 cells/mm3
lower in case women compared with control women, but this difference
was not statistically significant. |
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At
2 years and 4 years after starting ART, women who developed cervical
cancer had CD4 counts about 100 cells/mm3 and 160 cells/mm3 lower
than control women, respectively, both of which were significant. |
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Mean
CD4 counts of control women increased by an average of 8 cells/mm3
more per month than those of women who developed cervical cancer
during the year following ART initiation (P < 0.01) |
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HIV
viral load was not a significant predictor of cervical cancer. |
Taken
together, the investigators concluded, "the data suggest that combination
ART exhibits no effect on the incidence of anal HPV infection, no effect
on the incidence of anal SIL, [and] no restoration of anti-HPV T-cell
responses."
These
data suggest that HIV-positive MSM remain at risk of anal SIL despite
immune restoration, they added, a finding in accordance with several
epidemiological studies showing no significant decreases -- or even
increases -- in the occurrence of anal cancer among HIV positive men
in the ART era.
The researchers
recommended that HIV positive men -- whether on or off ART -- should
be screened for anal cancer, much as women receive regular Pap smears
or HPV tests to detect early signs of cervical cancer.
Cervical
Cancer in Women
In the
second study, Alison Abraham and fellow investigators with the NA-ACCORD
(North American AIDS Cohort Collaboration on Research and Design) study
looked at development of invasive cervical cancer -- the most severe
stage -- among women with HIV after ART initiation.
Some prior studies have found that while HIV positive women are more
likely to have high-risk HPV infection and precancerous cell changes,
frank invasive cervical cancer and related death are not significantly
more common compared with the general population in high-income countries
like the U.S. Researchers have suggested this is likely due to the fact
that HIV positive women typically receive regular screening that catches
cervical cell changes at an early more treatable stage.
This nested case-control analysis included some 110,000 HIV positive
women enrolled in the NA-ACCORD IeDEA database from 13 cohorts in North
America who started ART during follow-up. The median age was 40 years,
more than half were African-American, and about one-third had a history
on injection drug use.
Women
who developed invasive cervical cancer (cases) were matched to women
without invasive cancer (controls) according to age, time of ART initiation,
CD4 count, calendar period, cohort, and length of follow-up. The investigators
compared trends in average CD4 count at various time points prior to
invasive cancer diagnosis, starting 4 years before ART initiation.
Results
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CD4 cell count rose from about 300 cells/mm3 at study entry to 500
cells/mm3 at month 12. |
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Median
viral load fell from 4.8 to 1.6 log and more than 90% achieved undetectable
HIV RNA < 50 copies/mL. |
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Overall,
anal SIL did not regress despite CD4 cell gains after starting ART. |
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Prevalence
of SIL was similar at baseline and at month 12: |
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Anal
SIL overall: 54% at baseline vs 58% at month 12; |
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Low-grade
SIL: 32% vs 34%, respectively; |
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High-grade
SIL: 8% vs 14%, respectively. |
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Participants
continued to show evidence of overall and high-risk HPV infection
after ART initiation: |
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Any
HPV type: 97% at baseline vs 94% at month 12; |
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Any
high-risk HPV type: 92% at baseline vs 89% at month 12; |
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HPV-16:
40% vs 34%, respectively; |
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HPV-18:
18% vs 16%, respectively. |
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Both
at baseline and at month 12, participants had a median 5 types of
HPV overall and a median 3 high-risk types. |
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Among
29 participants who started out with normal cytology and histology
findings at baseline, 44% progressed to anal SIL at month 12. |
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Conversely,
among 41 men with anal SIL at baseline, 49% experienced some degree
of SIL regression and 32% achieved normal histology by month 12. |
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Participants
also did not clear infection with high-risk HPV-16 despite immune
restoration on ART. |
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No
significant changes in CD4 or CD8 T-cell responses to HPV were observed. |
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Specific
anti-HPV CD4 T-cell responses were mostly undetectable both at baseline
and at month 12. |
Based
on these findings, the investigators concluded that in this large North
American cohort, "average CD4 counts were consistently lower over
time for women who developed invasive cervical cancer than for similar
women who remained free of invasive cervical cancer over follow-up."
"These differences in CD4 trajectory between cases and controls
suggest a role of long-term immunosuppression," they continued.
Less robust CD4 cell recovery following ART was not explained by differences
in viral load (suggesting poorer adherence) or prior suboptimal use
of NRTIs (suggesting drug resistance).
Investigator affiliations:
Piketty study: Hopital Européen Georges Pompidou, Paris, France;
INSERM U943 - UPMC UMR S943, Paris, France; Hopital Lariboisiere, Paris,
France; Hopital Saint Antoine, Paris, France; Hopital de La Pitie-Salpetriere,
Paris, France; Hopital Bichat-Claude Bernard, Paris, France.
Abraham study: Johns Hopkins Bloomberg School of Public Health, Epidemiology,
Baltimore, MD; Harvard University, Boston, MA; Centers for Disease Control
and Prevention, Atlanta, GA; Yale University, New Haven, CT; University
of North Carolina, Chapel Hill, NC; Johns Hopkins School of Medicine,
Baltimore, MD; University of Calgary, Calgary, Canada; University of
California at San Francisco, San Francisco, CA; BC Centre for Excellence
in HIV/AIDS, Vancouver, Canada; University of Washington, Seattle, WA;
McGill University, Montreal, Canada; University of Toronto, Toronto,
Canada; Kaiser Permanente Northern California, Oakland, CA.
8/24/10
References
C Piketty,
A Si-Mohamed, E Lanoy, and others (Valparaiso Study Group). Lack of
regression of anal squamous intraepithelial lesions and anal HPV infections
despite immune restoration under cART. XVIII International AIDS Conference
(AIDS 2010). Vienna, February 18-23, 2010. Abstract
WEAB0103.
AG Abraham,
S Gange, Y Jing, and others (North American AIDS Cohort Collaboration
on Research and Design). CD4 count trajectories of HIV infected women
in North America with cervical cancer after initiating ART. XVIII International
AIDS Conference (AIDS 2010). Vienna, February 18-23, 2010. Abstract
WEAB0104.
