Maternal malaria and perinatal HIV transmission, Western Kenya (1,2).To determine whether maternal placental placental pertaining to or emanating from placenta. placental barrier the placental separation of maternal and fetal blood which varies in its structure and permeability between the species. malaria is associated with an increased risk for perinatal mother-to-child HIV HIV (Human Immunodeficiency Virus), either of two closely related retroviruses that invade T-helper lymphocytes and are responsible for AIDS. There are two types of HIV: HIV-1 and HIV-2. HIV-1 is responsible for the vast majority of AIDS in the United States. transmission (MTCT MTCT Mother to Child Transmission MTCT Manipulator/Teleoperator Control Technology MTCT Memphis Through Cairo Terms (barge freight on cargo originating on this stretch of the Mississippi River) MTCT Modified Truncated Cone Target ), we studied HIV-positive women in western Kenya. We enrolled 512 mother-infant pairs; 128 (25.0%) women had placental malaria, and 102 (19.9%) infants acquired HIV perinatally. [Log.sub.10] HIV viral load HIV viral load AIDS A measure of the amount of HIV RNA in blood, expressed as number of copies/mL of plasma. See AIDS, HIV. and episiotomy Episiotomy Definition An episiotomy is a surgical incision made in the area between the vagina and anus (perineum). This is done during the last stages of labor and delivery to expand the opening of the vagina to prevent tearing during the delivery of or perineal perineal /peri·ne·al/ (-ne´al) pertaining to the perineum. Perineal The diamond-shaped region of the body between the pubic arch and the anus. tear were associated with increased perinatal HIV transmission, whereas low-density placental malaria (<10,000 parasites/[micro]L) was associated with reduced risk (adjusted relative risk [ARR ARR See: Average rate of return ] 0.4). Among women dually infected with malaria and HIV, high-density placental malaria ([greater than or equal to]10,000 parasites/[micro]L) was associated with increased risk for perinatal MTCT (ARR 2.0), compared to low-density malaria. The interaction between placental malaria and MTCT appears to be variable and complex: placental malaria that is controlled at low density may cause an increase in broad-based immune responses that protect against MTCT; uncontrolled, high-density malaria may simultaneously disrupt placental architecture and generate substantial antigen stimulus to HIV replication and increase risk for MTCT. ********** Malaria during pregnancy is a serious problem in sub-Saharan Africa, affecting an estimated 24 million pregnant women; malaria prevalence may exceed 50% among primigravid and secundigravid women in malaria-endemic areas (1). During the past 2 decades, HIV and AIDS have emerged as major problems in many malaria-endemic areas of sub-Saharan Africa, where an estimated 28 million persons are infected with HIV (2). Sub-Saharan Africa accounts for more than two thirds of the world's 40 million HIV-infected persons and 80% of the world's HIV-infected women, with HIV prevalence rates sometimes exceeding 40% among pregnant women (3). Without intervention, as many as 30%-45% of pregnant women infected with HIV will pass the virus to their children through mother-to-child transmission mother-to-child transmission Vertical transmission, see there (MTCT) (4), of which 15%-30% is intrauterine intrauterine /in·tra·uter·ine/ (-u´ter-in) within the uterus. in·tra·u·ter·ine adj. Within the uterus. Intrauterine Situated or occuring in the uterus. or intrapartum. Given the wide overlap between areas where HIV and malaria are each prevalent, the epidemic of HIV/AIDS HIV/AIDS Human Immunodeficiency Virus/Acquired Immune Deficiency Syndrome in areas where Plasmodium falciparum Plasmodium fal·cip·a·rum n. A protozoan that causes falciparum malaria. is endemic has generated concern about potential interactions between the two infections, especially in sub-Saharan Africa (5-9). Studies have shown increased HIV replication both in blood mononuclear mononuclear /mono·nu·cle·ar/ (-noo´kle-er) 1. having but one nucleus. 2. a cell having a single nucleus, especially a monocyte of the blood or tissues. mon·o·nu·cle·ar adj. cells exposed to malaria antigens in vitro in vitro /in vi·tro/ (in ve´tro) [L.] within a glass; observable in a test tube; in an artificial environment. in vi·tro adj. In an artificial environment outside a living organism. (10) and in transgenic mice infected with P. chabaudi (11). Proviral loads are also higher among HIV-infected persons with clinical malaria compared to those without malaria; these levels remain high for at least 4 weeks after treatment (12). Although malaria may increase viral replication Viral replication is the term used by virologists to describe the propagation of biological viruses during the infection process in the target host cells. When used in the strictest sense, the term refers specifically to the amplification of the viral genome in the short term, the concern that the malaria-associated increase in viral replication may accelerate HIV disease progression has not been proven (13). Studies among pregnant women in sub-Saharan Africa have provided the first evidence of an important public health problem arising from the interaction of HIV and malaria. HIV infection appears to impair malarial immunity among pregnant women, as pregnant women infected with HIV demonstrate more frequent and higher density parasitemia parasitemia /par·a·si·te·mia/ (par?ah-si-te´me-ah) the presence of parasites, especially malarial forms, in the blood. par·a·si·te·mi·a n. The presence of parasites in the blood. than pregnant women not infected with HIV (5-7,14). More recent case-control (15) and longitudinal (16,17) studies on the clinical pattern of malaria in HIV-infected, nonpregnant women have shown HIV infection to be associated with an increased frequency of clinical malaria and parasitemia, particularly among persons with advanced HIV disease. Data from Malawi (18) have suggested that infants exposed in utero in utero (in u´ter-o) [L.] within the uterus. in u·ter·o adj. In the uterus. in utero adv. to both placental malaria and maternal HIV infection have an increased risk for postneonatal death three- to eightfold eightfold Adjective 1. having eight times as many or as much 2. composed of eight parts Adverb by eight times as many or as much Adj. 1. higher than infants born to mothers with either infection alone. We examined the relationship between placental malaria and perinatal HIV transmission in an area of western Kenya with high prevalence of malaria and HIV infection. Participants and Methods Study Site This study was conducted at Nyanza Provincial General Hospital (NPGH), a large publicly funded hospital in Kisumu (population 300,000) in western Kenya. Malaria transmission within Kisumu town is perennial, and P. falciparum is the predominant species, accounting for 98% of malaria cases (19). Chloroquine chloroquine /chlo·ro·quine/ (klor´o-kwin) an antiamebic and anti-inflammatory used in the treatment of malaria, giardiasis, extraintestinal amebiasis, lupus erythematosus, and rheumatoid arthritis; used also as the hydrochloride and resistance is prevalent in the area: 75%-80% of P. falciparum strains show a RII/RIII resistance pattern (20). The prevalence of HIV infection among pregnant women is approximately 25% (6,21). Recruitment and Follow-up Pregnant women were enrolled from June 1996 through May 2000. Screening procedures have been described previously (21). Briefly, women at the antenatal clinic antenatal clinic n → clínica prenatal antenatal clinic n → service m de consultation prénatale antenatal clinic antenatal n were eligible for participation if they had an uncomplicated singleton pregnancy of [greater than or equal to]32 weeks' gestation (based on the fundal height Fundal height, or MacDonald's rule, is a measure of the size of the uterus used to assess fetal growth and development. It is measured from the top of the pubic bone to the top of the uterus in centimeters. It should match the fetus' gestational age in weeks within 1 to 3 cm, e.g. estimation), resided within the Kisumu municipality, and had no known underlying chronic illness. Following informed consent, a structured questionnaire was administered in the local language (Dholuo or Kiswahili) to obtain information on sociodemographic, health, and obstetric ob·stet·ric or ob·stet·ri·cal adj. Of or relating to the profession of obstetrics or the care of women during and after pregnancy. obstetrical, obstetric pertaining to or emanating from obstetrics. factors. A trained HIV counselor then counseled each woman, and a posttest post·test n. A test given after a lesson or a period of instruction to determine what the students have learned. counseling appointment was made. A blood sample was taken for HIV antibody HIV antibody A self antibody specifically directed against one or more proteins or antigens on the surface of HIV, which may be minimally protective against HIV testing, hemoglobin level, and malaria thick blood film. All screened women were encouraged to deliver at NPGH. In addition, nonscreened women who delivered at NGPH NGPH National Grand Prix Holdings, LLC were eligible for participation if they met study inclusion criteria
Inclusion criteria are a set of conditions that must be met in order to participate in a clinical trial. . Routine use of zidovudine zidovudine /zi·do·vu·dine/ (zi-do´vu-den) a synthetic nucleoside (thymidine) analogue that inhibits replication of some retroviruses, including the human immunodeficiency virus; used in the treatment of HIV infection and AIDS. or nevirapine nevirapine /ne·vir·a·pine/ (ne-vir´ah-pen) a nonnucleoside inhibitor of HIV-1reverse transcriptase, used in combination with other antiretroviral agents in the treatment of HIV infection. was not the Kenyan Ministry of Health policy during the study period, and these drugs were not available in Ministry of Health facilities. At delivery, information was collected on mode and outcome of delivery and any illness and treatment in the previous 2 weeks. Within 24 hours of birth, infants were weighed ([+ or -]1 g) on an electronic balance (Ohaus, Florham Park, NJ), and gestational age ges·ta·tion·al age n. See estimated gestational age. Gestational age The estimated age of a fetus expressed in weeks, calculated from the first day of the last normal menstrual period. was assessed by using the Ballard method (22). All live, singleton, vaginally delivered infants of HIV-positive mothers were eligible for study. Infants were seen monthly until 12 months of age. Informed consent was obtained from all women before they were enrolled in this study. Human subjects guidelines of the Centers for Disease Control and Prevention Centers for Disease Control and Prevention (CDC), agency of the U.S. Public Health Service since 1973, with headquarters in Atlanta; it was established in 1946 as the Communicable Disease Center. (CDC See Control Data, century date change and Back Orifice. CDC - Control Data Corporation ) and the Kenya Medical Research Institute The Kenya Medical Research Institute (KEMRI) is one of East Africa's leading medical research centres. It is located in Kenya's capital, Nairobi. Established in 1979, KEMRI has played an important role in the fight against malaria, HIV/AIDS and other diseases in Kenya, and ethical review committee were strictly followed. Mothers of enrolled infants signed an additional informed consent form for infant participation. Ethical Review The study protocol was approved in 1995 by the institutional review boards of the Kenya Medical Research Institute; CDC, Atlanta, Georgia, USA; and the Academic Medical Center (AMC (Advanced Mezzanine Card) See AdvancedTCA. ), University of Amsterdam, Amsterdam, The Netherlands, and was reviewed annually by the participating institutions. This study occurred during a changing environment in preventing perinatal HIV transmission, with results of studies in other countries demonstrating the benefits of short-course AZT AZT or zidovudine (zīdō`vy  dēn'), drug used to treat patients infected with the human immunodeficiency virus (HIV), which causes AIDS; also called use (23,24) or nevirapine use (25) in late pregnancy and perinatally
to reduce the risk for MTCT. Similarly, studies of malaria prevention in
pregnancy during the study interval were demonstrating the benefit of
intermittent antimalarial antimalarial /an·ti·ma·lar·i·al/ (-mah-lar´e-al) therapeutically effective against malaria, or an agent with this quality. an·ti·ma·lar·i·al adj. Preventing or relieving the symptoms of malaria. treatment to prevent maternal anemia and low birth weight (6,26). The participating institutions and the Kenyan Ministry of Health were engaged in discussions about these findings regarding the ethical considerations for this investigation. The study continued with full ethical approvals during these discussions. Investigators and institutions have supported the transition to a system that supports providing intermittent preventive antimalarial therapy during pregnancy, according to according to prep. 1. As stated or indicated by; on the authority of: according to historians. 2. In keeping with: according to instructions. 3. the adopted Kenyan national policy. The MTCT prevention program now offers HIV counseling and testing, community education, and antiretroviral drugs Antiretroviral Drugs Definition Antiretroviral drugs inhibit the reproduction of retroviruses—viruses composed of RNA rather than DNA. The best known of this group is HIV, human immunodeficiency virus, the causative agent of AIDS. to prevent MTCT in the study setting (4). Blood Sampling and Laboratory Procedures At delivery, maternal peripheral and placental thick blood films were prepared, stained with 10% Giemsa, and examined under oil immersion for malaria parasites. Placental blood was obtained by cutting into the maternal side of the placenta placenta (pləsĕn`tə) or afterbirth, organ that develops in the uterus during pregnancy. It is a unique characteristic of the higher (or placental) mammals. In humans it is a thick mass, about 7 in. and placing collected blood on a slide. A thick film was considered negative if 100 microscopic fields showed no parasites. Malaria parasites and leukocytes were counted in the same fields until 300 leukocytes were counted. Parasite densities were estimated by using an assumed count of 8,000 leukocytes/[micro]L blood. Blood samples were collected into EDTA EDTA: see chelating agents. tubes. At delivery, blood was collected from mothers of enrolled infants to assess viral load viral load n. The concentration of a virus, such as HIV, in the blood. viral load, n a measure of the number of virus particles present in the bloodstream, expressed as copies per milliliter. , whether syphilis was present, and hemoglobin level. One month postpartum, maternal venous blood venous blood n. Abbr. v Blood that has passed through the capillaries of various tissues other than the lungs, is found in the veins, in the right chambers of the heart, and in pulmonary arteries, and is usually dark red as a result of a was collected to determine counts of CD4-and CD8-positive T-lymphocytes (CD4+ and CD8+). Capillary blood was collected from infants by a heel prick on the day of delivery and then monthly thereafter for HIV testing. Plasma was separated from blood samples and stored at -70[degrees]C. Infant HIV testing was done by polymerase chain reaction polymerase chain reaction (pŏl`ĭmərās') (PCR), laboratory process in which a particular DNA segment from a mixture of DNA chains is rapidly replicated, producing a large, readily analyzed sample of a piece of DNA; the process is (PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) ) of proviral DNA DNA: see nucleic acid. DNA or deoxyribonucleic acid One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes. extracted from peripheral blood peripheral blood Cardiology Blood circulating in the system/body mononuclear cells (27). HIV testing of pregnant women used two rapid test methods: an initial Serostrip HIV-1/2 (Saliva Diagnostic Systems Pte Ltd PTE LTD Private Limited , Singapore) and a confirmatory Capillus HIV-1/HIV-2 (Cambridge Diagnostics, Wicklow, Ireland) on all Serostrip-positive samples. Sequential testing of samples using both methods has a high sensitivity and specificity (Richard W. Steketee, pers. comm.). Western blot Western blot A technique developed in 1979 that is used to confirm ELISA results. HIV antigen is purified by electrophoresis and attached by blotting to a nylon or nitrocellulose filter. was performed on discordant samples. Maternal CD4+ and CD8+ counts were assessed by using commercial, dual-label monoclonal antibodies This is a list of monoclonal antibodies, antibodies which are clones of a single parent cell. When used as medications, the generic names end in -mab (see "Nomenclature of monoclonal antibodies"). (Becton-Dickinson Immunocytometry, San Jose San Jose, city, United States San Jose (sănəzā`, săn hōzā`), city (1990 pop. 782,248), seat of Santa Clara co., W central Calif.; founded 1777, inc. 1850. , CA) and standard fluorescent-activated cell sorting (FACScan, Becton-Dickinson) analysis following whole-blood lysis lysis /ly·sis/ (li´sis) 1. destruction or decomposition, as of a cell or other substance, under influence of a specific agent. 2. mobilization of an organ by division of restraining adhesions. 3. (28). Maternal HIV-1 viral load was determined by the Roche Amplicor HIV-1 monitor test version 1.0 (Roche Diagnostics Roche Diagnostics Division is a subsidiary of Hoffmann-La Roche which manufactures equipment and reagents for research and medical diagnostic applications. Internally, it is organized into six major business areas: Roche Applied Science, Roche Centralized Diagnostics, Roche , Indianapolis, IN), with a quantification limit of 400 viral copies per milliliter milliliter /mil·li·li·ter/ (mL) (-le?ter) one thousandth (10-3) of a liter. mil·li·li·ter n. Abbr. . Syphilis antibodies were detected by venereal disease venereal disease (vənēr`ēəl): see sexually transmitted disease. research laboratory (VDRL VDRL Venereal Disease Research Laboratory. VDRL n. A flocculation test for syphilis, using cardiolipin-lecithin-cholesterol antigen as developed by the Venereal Disease Research Laboratory, a former federal facility. ) slide test (EUROTEX-VDRL, Euromedi equip ltd., West Harrow West Harrow is an area in the London Borough of Harrow. Location As its name suggests, West Harrow is located on the western side of the London Borough of Harrow, and roughly halfway between the north and south boundaries of the borough. , UK). Hemoglobin was measured to the nearest 0.1 g/dL using a Hemocue machine (Mission Viejo, CA). Definitions An uncomplicated pregnancy was defined as a pregnancy without the presence of AIDS-defining symptoms, hypertension, preeclampsia preeclampsia /pre·eclamp·sia/ (pre?e-klamp´se-ah) a toxemia of late pregnancy, characterized by hypertension, proteinuria, and edema. pre·e·clamp·si·a n. , polyhydramnios, abnormal fetal presentation, history of a cesarean section cesarean section (sĭzâr`ēən), delivery of an infant by surgical removal from the uterus through an abdominal incision. The operation is of ancient origin: indeed, the name derives from the legend that Julius Caesar was born in this , hemorrhage, or repeated spontaneous abortions (>2). Placental parasitemia was defined as any plasmodial plas·mo·di·al adj. Relating to a plasmodium or a species of the genus Plasmodium. asexual asexual /asex·u·al/ (a-sek´shoo-al) having no sex; not sexual; not pertaining to sex. a·sex·u·al adj. 1. Having no evident sex or sex organs; sexless. 2. form detected on a thick film. Maternal HIV infection was defined as a positive result on both rapid tests; women not reactive with the initial Serostrip HIV-1/2 test were considered HIV uninfected. Women whose serostatus could not be determined (i.e., those with discordant results on the two rapid tests and an indeterminate status with Western blot) were excluded from analysis. Newborns were classified as normal birth weight if they weighed [less than or equal to]2,500 g, regardless of gestational age, and low birth weight if they weighed <2,500 g. Preterm preterm /pre·term/ (-term´) before completion of the full term; said of pregnancy or of an infant. pre·term adj. delivery was defined as occurring at <37 weeks of gestation. Small for gestational age small for gestational age Intrauterine growth retardation Neonatology adjective Referring to an infant whose gestational age and weight gain are < expected for age. See Low birthweight. was defined as sex-specific birth weight [less than or equal to]10th percentile for weight-for-gestational-age (29). Determining Infant HIV Status An algorithm was developed to describe the perinatal HIV infection status of infants. Infants were classified as having acquired HIV infection perinatally (e.g., in utero or during labor and delivery) if they met the following conditions: 1) died and by the time of death had [greater than or equal to]2 consecutive positive HIV PCR tests, the first of which was at [less than or equal to]4 months of age; 2) were lost to follow-up but had had [greater than or equal to]3 consecutive positive PCR results, the first of which was at [less than or equal to]4 months of age; 3) remained alive with continued and consistent positive PCR results, the first of which was at [less than or equal to]4 months of age. Infants were considered negative for perinatally acquired HIV if they had [greater than or equal to]3 PCR tests performed on them, and all tests were negative, with at least one of the negative tests at [greater than or equal to]4 months of age. Because infants had to be [greater than or equal to]4 months old to be classified as uninfected, those who died or were lost to follow-up before 4 months of age were excluded. Infants who acquired HIV at [greater than or equal to]5 months of age were considered to have acquired HIV postnatally and were included as nontransmitters from the perinatal perspective. Infants for whom we had insufficient PCR data to determine their status were classified as indeterminate and were excluded. Mothers of infected infants were classified as transmitters and those of uninfected infants as nontransmitters. Data Analysis and Statistical Methods Univariate Analysis Plasma virus levels load below the limit of quantification (400 copies/[micro]L) were assigned a value of 200 copies/[micro]L; plasma viral load results were then [log.sub.10]-transformed. We defined high-density placental parasitemia as [greater than or equal to] 10,000 parasites/[micro]L, which corresponded approximately to the uppermost quintile quin·tile n. 1. The astrological aspect of planets distant from each other by 72° or one fifth of the zodiac. 2. Statistics The portion of a frequency distribution containing one fifth of the total sample. of parasite density. Univariate analyses were performed by using [chi square chi square (kī), n a nonparametric statistic used with discrete data in the form of frequency count (nominal data) or percentages or proportions that can be reduced to frequencies. ] or Fisher exact tests (for cross-tabulations with an expected value Expected value The weighted average of a probability distribution. Also known as the mean value. in any cell [less than or equal to]5) to compare proportions for categorical variables; t tests were used to compare normally distributed continuous variables. Relative risks (RRs) were computed with their 95% confidence interval confidence interval, n a statistical device used to determine the range within which an acceptable datum would fall. Confidence intervals are usually expressed in percentages, typically 95% or 99%. (CI) to measure the strength of the associations between potential risk factors and perinatal MTCT. Multivariate Analysis multivariate analysis, n a statistical approach used to evaluate multiple variables. multivariate analysis, n a set of techniques used when variation in several variables has to be studied simultaneously. To evaluate the effect of placental malaria on perinatal MTCT, a Poisson log-linear model log-linear model a statistical model which models frequency counts in contingency tables by using an analysis of variance approach. containing placental malaria and maternal viral load as primary predictor variables was constructed by using backward elimination; adjusted RRs were computed. An interaction term between placental malaria density and maternal viral load was significant (p = 0.02) and was retained in the model. Because women with and without placental malaria may have different risk factors for perinatal MTCT, we fit three separate multivariate models: all study women, women without placental malaria, and women with placental malaria. All tests were two-sided; p values <0.05 were considered significant. Analysis was done using STATA (StataCorp. 2001. Stata Statistical Software: Release 7.0 College Station, TX) and SAS (1) (SAS Institute Inc., Cary, NC, www.sas.com) A software company that specializes in data warehousing and decision support software based on the SAS System. Founded in 1976, SAS is one of the world's largest privately held software companies. See SAS System. (Version 8.0, SAS Institute, Cary, NC). Results Study Population A total of 829 mother-infant pairs were enrolled; 317 (38.2%) infants with incomplete follow-up or indeterminate HIV status were excluded, leaving 512 mother-infant pairs. Included and excluded women did not differ in age, level of education, mean maternal viral load, mean CD4+ counts, malaria rates, high-density malaria rates, proportion of low birth order (i.e., gravida [less than or equal to]2 versus [greater than or equal to]3), and rates of episiotomy or perineal tear. However, excluded women were more likely to have infants born with low birth weight (9.1% versus 5.5%, p = 0.04). The baseline characteristics of the 512 women included in the analysis are shown in Table 1. Among these 512 women, 128 (25.0%) had placental malaria and 353 (84.4%) had anemia (hemoglobin <11 g/dL). Correlates of Perinatal MTCT Of 512 mothers, 102 (19.9%) transmitted HIV to their infants perinatally. High maternal viral load ([greater than or equal to] 10,000 viral copies/[micro]L) and low CD4+ count (<200 cells/[micro]L) were significantly associated with perinatal MTCT (Table 2). When analyzed as continuous variables, transmitting mothers had higher geometric mean (mathematics) geometric mean - The Nth root of the product of N numbers. If each number in a list of numbers was replaced with their geometric mean, then multiplying them all together would still give the same result. viral loads than nontransmitting mothers (7,083 versus 1,378 copies/[micro]L; p<0.001) and low mean CD4+ count (511 versus 657 cells/[micro]L; p<0.001). Other characteristics significantly associated with perinatal MTCT included episiotomy or perineal tear, low birth weight or small-for-gestational-age infants, and being of low birth order (primigravid or secundigravid). Maternal peripheral parasitemia at delivery was not associated with MTCT; however, placental malaria was associated with a 40% reduction in the risk for perinatal MTCT (RR 0.6, 95% CI 0.4 to 1.0, p = 0.05) (Table 2). Compared to women without placental malaria (perinatal MTCT rate = 21.9%), women with placental parasitemia at lower densities (<10,000 parasites/[micro]L) had a lower rate of perinatal MTCT (11.5%); this was not true for women with higher-density placental parasitemia ([greater than or equal to] 10,000 parasites/[micro]L, perinatal MTCT rate = 25.0%), who represented approximately one fifth of women with placental malaria. Among women with viral load below the detection level, perinatal MTCT occurred in none of 35 mothers with malaria, compared to 10 (8.7%) of 115 mothers without malaria (p = 0.12). Multivariate Analysis of Risk Factors for Perinatal MTCT Among all study women, high maternal viral load and episiotomy or perineal tear were independent risk factors, and low-density (but not high-density) malaria was an independent protective factor for perinatal MTCT. Among women without microscopically detectable placental malaria, high maternal viral load, gravidity gravidity Obstetrics The state of being, or having been, pregnant. Cf Gravity. [less than or equal to]2, and low birth weight in the newborn were significant risk factors or markers for perinatal MTCT. Among women with placental malaria (where perinatal MTCT was overall lower than in the malaria-negative women), high maternal viral load, episiotomy or perineal tear, and high-density placental infection were significant risk factors for perinatal MTCT (Table 3). In both the multivariate models for the entire population and women with placental malaria, significant interaction was found between viral load and placental malaria density. In further examination of the interaction between maternal viral load and placental malaria, we found no significant differences in the frequency of episiotomy or perineal tear, mean CD4+ count, mean maternal hemoglobin level, mean birth weight, and frequency of small-for-gestational-age neonates among women without malaria, those with low-density placental malaria, and those with high-density placental malaria. Women with placental malaria were of lower mean gravidity than women without malaria (2.1 vs. 2.4, p = 0.03). Geometric mean maternal viral load was slightly higher in women with low-density placental malaria (2,226 copies/[micro]L) and was nearly twofold higher in women with high-density placental malaria (3,390 copies/[micro]L) than the viral load in women without placental malaria (1,774 copies/[micro]L); however, these differences were not significant (p = 0.14). Viral load was significantly higher among women with peripheral malaria parasitemia at delivery (2,979 copies/[micro]L) than among women without (1,725 copies/[micro]L, p = 0.03). As shown in Table 4, the geometric mean viral load was five-fold higher in transmitters than in nontransmitters. While in women without placental malaria the geometric mean viral load in transmitters was fourfold higher than in nontransmitters, among women with malaria, the geometric mean viral load was 25-fold higher in transmitters than in nontransmitters. Among transmitting women, those with placental malaria had an eightfold higher geometric mean viral load than those women without placental malaria. These associations were further evaluated in models comparing the relative risk for perinatal transmission between the three groups with placental malaria at various levels of maternal viral load. Low-density placental parasitemia was associated with significant protection for perinatal MTCT at the lower viral load levels, but not at higher viral load levels (Figure 1). When women with low- and high-density parasitemia were compared (Figure 2), high-density placental parasitemia was associated with increased risk for perinatal MTCT but only at the higher viral load levels. Discussion This evaluation of perinatal HIV transmission in a malarious area of western Kenya demonstrated that approximately 20% of infants born to HIV-infected mothers acquired HIV by 4 months of age, similar to rates reported in other sub-Saharan African settings (30-32). Consistent with other studies, we found that maternal viral load in peripheral blood at the time of delivery and having an episiotomy or perineal tear were risk factors for perinatal MTCT (33,34). Contrary to our expectations, we observed that women with placental malaria had lower rates of perinatal MTCT than women without placental malaria. However, women with high-density malaria had significantly higher rates of perinatal MTCT than parasitemic women with low-density malaria. In additional models, only low placental parasite density (1-9,999 parasites/[micro]L of blood) was associated with protection from perinatal MTCT; high-density placental infection was either a risk factor for perinatal MTCT (in the model evaluating only women with malaria) or it was a neutral factor (in the model evaluating all women). Maternal viral load was slightly higher in women with high-density placental malaria, and, among transmitting women, mean viral load was eightfold higher if the woman had concurrent placental malaria, consistent with the suggestion that high-density malaria may be an important stimulus of viral replication (10-12). Our study had some important limitations. First, only healthy women were screened for this study; no women with AIDS or any known underlying chronic illness were enrolled. Although this eliminated potential conditions that could have complicated the analysis (e.g., a higher likelihood of additional concurrent infections), it restricted our study population to the "healthiest" women with HIV and likely resulted in an underestimate of the overall rate of perinatal MTCT in our study area. Some infants categorized as having acquired HIV through perinatal transmission may have actually acquired it through early breastfeeding transmission. However, including these infants would likely bias the results toward underestimating the magnitude of the observed risks. Our measurement of placental malaria was limited to microscopy examination of placental smears and could have been inexact in·ex·act adj. 1. Not strictly accurate or precise; not exact: an inexact quotation; an inexact description of what had taken place. 2. ; those with no evidence of malaria may have had very low-density infection and may have been misclassified as having no malaria. Such misclassification would be expected to bias our findings toward the null hypothesis null hypothesis, n theoretical assumption that a given therapy will have results not statistically different from another treatment. null hypothesis, n . Because placental malaria can cause an inflammatory response in the placenta, the use of leukocyte count leukocyte count see White cell count to calculate parasite density may have resulted in an underestimation. However, our cutoff of 10,000 parasites/[micro]L for high-density placental parasitemia is essentially a relative measure based on the upper quintile of densities; therefore, we do not think that our estimation technique would have introduced any bias. Finally, in a study such as ours, loss to follow-up always has the potential to introduce bias. Approximately one third of infants enrolled in our study were lost to follow-up. However, as noted, these mothers and infants were generally similar to the study population included in our analysis, and we were unable to detect biases that would have affected our analysis. Our observation of an association between low-density placental malaria and reduced perinatal MTCT has several possible explanations. First, over 16% of women reported self-treatment (typically for fever) with chloroquine during pregnancy. High-grade chloroquine resistance in this area is widespread; its use is unlikely to clear placental infections, but it may reduce parasite densities. Chloroquine is known to have anti-HIV properties and to reduce HIV-1 replication and viral loads in adults (35,36) and as such could potentially reduce the risk for perinatal MTCT. Although we identified no differences in the proportion of women with or without placental malaria who used chloroquine, and no association was found between chloroquine usage and MTCT, women identified as having placental malaria may have used chloroquine more frequently and at higher doses (information that was not collected) than women without placental malaria. A second possibility is that some of the women classified as having placentas negative for malaria parasites may actually have had low-level chronic malaria chronic malaria n. Malaria that develops after repeated attacks of one of the acute forms, usually falciparum malaria, and is characterized by profound anemia, enlargement of the spleen, emaciation, mental depression, sallow complexion, edema of the associated with inflammation and increased HIV replication. In contrast, women classified as having low-density malaria may have had recent malaria with minimal inflammatory response and thus no increase in HIV replication. Unfortunately, blood films are not capable of detecting inflammatory responses. A more likely explanation is that a balance exists in the uterine-placental-fetal environment among malaria-induced antigen stimulation, HIV viral replication, maternal host immune response to both malaria and HIV, and the likelihood of MTCT. Although high viral load has been shown to increase the risk for MTCT, no more than half of exposed infants, even at high maternal viral load, become infected with HIV-1. These data suggest that other systemic or placental factors must be important in preventing HIV-1 transmission. Recent studies suggest that selected cytokines Cytokines Chemicals made by the cells that act on other cells to stimulate or inhibit their function. Cytokines that stimulate growth are called "growth factors. and hormones potentially affect HIV-1 transplacental transplacental /trans·pla·cen·tal/ (-plah-sen´tal) through the placenta. trans·pla·cen·tal adj. Relating to or involving passage through or across the placenta. transmission and that both innate and acquired protection play a role in MTCT (37). First, malaria is known to induce disequilibrium disequilibrium /dis·equi·lib·ri·um/ (dis-e?kwi-lib´re-um) dysequilibrium. linkage disequilibrium in the balance between Th1 and Th2 responses, favoring the Th1 pathway (38-40). T-helper responses are known to control HIV replication; hence, inducing Th1 response in the placental compartment could lead to reduced HIV-1 replication (41,42). Indeed, a moderate increase was found in the Th1 cytokine Cytokine Any of a group of soluble proteins that are released by a cell to send messages which are delivered to the same cell (autocrine), an adjacent cell (paracrine), or a distant cell (endocrine). interferon-[gamma] response in the intervillous blood mononuclear cell responses of HIV-positive mothers with placental malaria as compared to HIV-positive mothers without placental malaria (43). Second, leukemia inhibitory factor Leukemia inhibitory factor, or LIF, an interleukin 6 class cytokine, is a chemical in cells that affects their growth and development. Function LIF derives its name from its ability to induce the terminal differentiation of myeloid leukaemic cells. induces a potent inhibition of HIV replication, and this cytokine is upregulated in placentas of women who do not transmit HIV (44). Malarial antigens may induce production of leukemia inhibitory factor that results in reduced rates of perinatal MTCT. Third, malarial antigen may result in altered chemokine chemokine /che·mo·kine/ (ke´mo-kin) any of a group of low molecular weight cytokines identified on the basis of their ability to induce chemotaxis or chemokinesis in leukocytes (or in particular populations of leukocytes) in inflammation. production, which in turn can block chemokine receptors necessary for cellular HIV entry (45). Recent immunologic studies conducted in a group of women who participated in this cohort showed that macrophage inflammatory protein This article is about proteins. For the chemical compound CCl4, see Carbon tetrachloride. Macrophage Inflammatory Proteins (MIP) belong to the family of chemotactic cytokines known as chemokines. (MIP MIP See: Monthly income preferred security )- 1[beta], a chemokine known to block the entry of HIV-1, was significantly elevated in the intervillous blood plasma blood plasma n. The yellow or gray-yellow, protein-containing fluid portion of blood in which the blood cells and platelets are normally suspended. of women with placental malaria irrespective of their HIV status. In women with concurrent HIV and placental malaria, the intervillous blood plasma levels of MIP-1[beta] were significantly elevated compared to HIV-negative women with placental malaria and HIV-positive women without placental malaria (46). Thus, a complex balance of antigen stimulus and immune response may occur in the placenta, as demonstrated in recent studies focusing on the placental intervillous blood responses (38-40,43,46). In this scenario, active placental malaria might lead to one of the local immune responses described. This response may control the density of parasitemia and may also provide immune control that limits perinatal MTCT. For most women with placental malaria (approximately 80% in our study), this resultant balance leads to "protection" with controlled (low-density) malaria and reduced perinatal MTCT. For a minority of women with malaria (approximately 20% in our study), the balance is tilted to inadequate control of placental malaria (i.e., higher density of malaria parasites with concomitant increased antigen stimulation of viral replication and higher viral load) and higher rates of perinatal MTCT. This finding is consistent with our observation that women with high-density placental malaria do have higher rates of perinatal MTCT than women with low-density placental malaria, but that they require much higher viral loads to achieve this transmission. Our findings suggest complex relationships between malaria, viral load, and perinatal MTCT. These findings will need to be confirmed and expanded upon in further research in different settings. The finding of reduced perinatal MTCT in the presence of low-density, but not high-density, placental malaria does not suggest altering existing recommendations for the use of intermittent preventive antimalarial treatment in pregnant women in malarious areas of Africa (47). For most dually (malaria and HIV) infected women, the overall outcome would have modest benefit in reducing perinatal MTCT, but for the minority with insufficiently controlled infections, perinatal MTCT would be increased. At this point, we cannot differentiate in advance which women will end up in which group. The important benefit of anti-malarial treatment may be to reduce the likelihood of women having high-density placental malaria and in also helping reduce the other known adverse effects of malaria during pregnancy, including anemia, low birth weight, and prematurity (1). As noted earlier, this study was carried out in Kenya in a changing environment of perinatal HIV and malaria prevention and has been transformed into a program delivering short-course antenatal an·te·na·tal adj. See prenatal. antenatal before parturition. Called also prenatal, antepartal. antiretroviral therapy to HIV-infected women and a system to support providing intermittent preventive antimalarial treatment during pregnancy according to the newly adopted national policy (48). As more countries adopt policies of antiretroviral and antimalarial interventions in pregnancy, the interrelationship in·ter·re·late tr. & intr.v. in·ter·re·lat·ed, in·ter·re·lat·ing, in·ter·re·lates To place in or come into mutual relationship. in and ultimate benefit of these two interventions need to continue to be evaluated. Acknowledgments We thank the project staff at the antenatal clinic, labor ward, counselors, laboratory technicians, and computer data entry staff for assisting in many ways to realize this work. We thank Kevin DeCock, Laurence Slutsker, and Venkatachalam Udhayakumar for their valuable comments on the manuscript; John Odondi, the medical superintendent, and health workers from the Nyanza Provincial General Hospital for their cooperation in the study; the Director of the Kenya Medical Research Institute for his permission to publish this work; and all the pregnant women and their infants for their participation in this study. This study was supported by grant number AOT AOT Agency of Transportation (Vermont, USA) AOT Ahead-of-Time AOT Assisted Outpatient Treatment AOT Aerosol Optical Thickness AOT All of Them (band) AOT As Opposed To AOT Among Other Things 0483-PH1-2171, HRN-A-00-04-00010-02 from the United States Agency for International Development The United States Agency for International Development (or USAID) is the U.S. government organization responsible for most non-military foreign aid. An independent federal agency, it receives overall foreign policy guidance from the U.S. and by The Netherlands Foundation for the Advancement of Tropical Research, The Hague, The Netherlands. (1) This work was presented in part at the Epidemic Intelligence Service The Epidemic Intelligence Service is a program of the United States' Centers for Disease Control and Prevention. Established in 1951 due to biological warfare concerns arising from the Korean War, it has become a hands-on two-year postgraduate training program in epidemiology, with Conference, Centers for Disease Control and Prevention, April 2001, Atlanta, GA. (2) Use of trade names is for identification only and does not imply endorsement by the Kenya Medical Research Institute or The Ministry of Health, Kenya, or by the Public Health Service, U.S. Department of Health and Human Services Noun 1. Department of Health and Human Services - the United States federal department that administers all federal programs dealing with health and welfare; created in 1979 Health and Human Services, HHS .
Table 1. Characteristics of HIV-positive women and their newborns
participating in perinatal HIV transmission study, Kisumu, western
Kenya, 1996-2001 (a)
Characteristic All women (N = 512) (b)
Maternal sociodemographic
Luo ethnicity 87%
Mean age (y) [+ or -] SD 22.4 [+ or -] 4.4
(range 14-39)
Mean gravidity [+ or -] SD 2.3 [+ or -] 1.4 (range 1-9)
Primigravid 35.9%
Completed primary education 68.0% (n = 510)
([greater than or equal to] 8 y)
No salaried employment 74.3%
Married 78.4%
History of fever and treatment for
malaria
History of fever previous week 23.2% (n = 509)
at screening
History of fever a fortnight 28.0% (n = 511)
before delivery
Treated with antimalarials in 30.9%
current pregnancy
Treated with chloroquine during 16.6%
current pregnancy
Axillary temperature [greater 2.9% (n = 455)
than or equal to]
37.5[degrees]C at screening
Laboratory
VDRL-positive 7.3% (n = 385)
Hemoglobin <11 g/dL at screening 84.4% (n = 418)
Hemoglobin <8 g/dL at screening 20.6% (n = 418)
Mean maternal CD4+ count (% <200 629 [+ or -] 334 (4.7%)
cells/[micro]L) 1 mo postpartum (n = 464)
Mean maternal [log.sub.10] viral 3.28 [+ or -] 0.92 (33.0%)
load at delivery (% below (n = 455)
detection limit of 400 copies)
Peripheral parasitemia at screening 21.9% (n = 415)
Peripheral parasitemia at delivery 19.7% (n = 497)
Placental malaria 25.0%
Delivery
Episiotomy or perineal tear 36.4%
Mean duration of rupture of 2.7 [+ or -] 6.2 (15.4%)
membranes [+ or -]
SD (% >4 hours)
Newborn
Mean birth weight (% low birth 3144 [+ or -] 420 (5.5%)
weight)
Prematurity (<37 wks completed 8.2%
gestation)
Maternal HIV transmitters 102 (19.9%)
(a) VDRL, venereal disease research laboratory slide test.
(b) If characteristic not measured for all 512 women, n is
given in parentheses.
Table 2. Risk factors associated with perinatal HIV infection by
maternal viral, immunologic, obstetric, and other factors (univariate
analysis), western Kenya, 1996-2001
No. infected
Variable No. studied (%)
Viral load >10,000
No 358 50 (14.0)
Yes 97 40 (41.2)
CD4+ cells <200
No 442 74 (16.7)
Yes 22 13 (59.1)
Hemoglobin <8 g/dL at screening
No 332 58 (17.5)
Yes 86 22 (25.6)
3rd-trimester maternal parasitemia
No 324 64 (19.8)
Yes 91 15 (16.5)
Maternal parasitemia at delivery
No 399 83 (20.8)
Yes 98 15 (15.3)
Placental malaria
No 384 84 (21.9)
Yes 128 18 (14.1)
Ever been treated for tuberculosis
No 496 98 (19.8)
Yes 13 4 (30.8)
Treated with chloroquine during pregnancy
No 427 88 (20.6)
Yes 85 14 (16.5)
Treated for vaginal discharge
No 477 93 (19.5)
Yes 32 9 (28.1)
Hospitalized during current pregnancy
No 472 95 (20.1)
Yes 39 7 (18.0)
History of fever 2 wks before delivery
No 368 70 (19.0)
Yes 143 32 (22.4)
Episiotomy or perineal tear
No 325 56 (17.2)
Yes 186 46 (24.7)
Primi- or secundigravid
No 190 26 (13.7)
Yes 322 76 (23.6)
Low birth weight
No 484 91 (18.8)
Yes 28 11 (39.3)
Prematurity
No 468 92 (19.7)
Yes 42 10 (23.8)
Small for gestational age
No 444 83 (18.7)
Yes 66 19 (28.8)
Relative risk
(95% confidence
Variable interval) p
Viral load >10,000
No
Yes 3.0 (2.1 to 4.2) <0.001
CD4+ cells <200
No
Yes 3.5 (2.4 to 5.3) <0.001
Hemoglobin <8 g/dL at screening
No
Yes 1.5 (1.0 to 2.3) 0.09
3rd-trimester maternal parasitemia
No
Yes 0.8 (0.5 to 1.4) 0.48
Maternal parasitemia at delivery
No
Yes 0.7 (0.4 to 1.2) 0.22
Placental malaria
No
Yes 0.6 (0.4 to 1.0) 0.05
Ever been treated for tuberculosis
No
Yes 1.6 (0.7 to 3.6) 0.33
Treated with chloroquine during pregnancy
No
Yes 0.8 (0.5 to 1.3) 0.38
Treated for vaginal discharge
No
Yes 1.7 (0.8 to 2.6) 0.24
Hospitalized during current pregnancy
No
Yes 0.9 (0.4 to 1.8) 0.74
History of fever 2 wks before delivery
No
Yes 1.2 (0.8 to 1.7) 0.39
Episiotomy or perineal tear
No
Yes 1.4 (1.0 to 2.0) 0.04
Primi- or secundigravid
No
Yes 1.7 (1.1 to 2.5) 0.007
Low birth weight
No
Yes 2.1 (1.3 to 3.4) 0.008
Prematurity
No
Yes 1.2 (0.7 to 2.1) 0.52
Small for gestational age
No
Yes 1.5 (1.0 to 2.4) 0.06
Table 3. Multivariate analysis of risk factors for perinatal
HIV transmission, western Kenya, 1996-2001
Adjusted relative risks
(ARR) for perinatal HIV
transmission (a)
All women, (b) N = 454
ARR (95% CI) p
[Log.sub.10] viral load 1.8 (1.6 to 2.1) <0.001
Episiotomy or perineal tear 1.6 (1.2 to 2.1) 0.004
Low birth weight --
Gravidity <3 versus [greater than or --
equal to]3
Placental malaria status
Negative Reference (c)
<10,000 parasites/[micro]L 0.4 (0.2 to 0.6) (b) <0.001
[greater than or equal to] 10,000 0.7 (0.3 to 21.5) (b) NS
parasites/[micro]L
Adjusted relative risks
(ARR) for perinatal HIV
transmission (a)
Placental
malaria-negative, n = 348
ARR (95% CI) p
[Log.sub.10] viral load 1.7 (1.4 to 2.0) <0.001
Episiotomy or perineal tear --
Low birth weight 1.9 (1.1 to 3.2) 0.03
Gravidity <3 versus [greater than or 1.8 (1.2 to 2.8) 0.003
equal to]3
Placental malaria status
Negative N/A
<10,000 parasites/[micro]L N/A
[greater than or equal to] 10,000 N/A
parasites/[micro]L
Adjusted relative risks
(ARR) for perinatal HIV
transmission (a)
Placental malaria-
positive, (b) n = 107
ARR (95% CI) p
[Log.sub.10] viral load 3.5 (2.5 to 4.8) <0.001
Episiotomy or perineal tear 4.8 (2.3 to 9.7) <0.001
Low birth weight --
Gravidity <3 versus [greater than or --
equal to]3
Placental malaria status
Negative
<10,000 parasites/[micro]L Reference
[greater than or equal to] 10,000 2.0 (1.1 to 3.9) 0.04
parasites/[micro]L
(a)-, factor was not returned in the final model; CI, confidence
interval; N/A, not applicable; NS, not significant.
(b) A significant interaction was found between viral load and
placental malaria density (p = 0.02) in these analyses. The effect
of this interaction on the relative risk for placental malaria is
shown in Figures 1 and 2. All relative risks given in this table do
not include this interaction but give a weighted average of the
malaria effect placental at various levels of vital load.
(c ) An alternative model, in which placental malaria was fit as a
binary variable (positive or negative), showed that placental malaria
was protective for perinatal HIV transmission (relative risk 0.4,
95% CI 0.3 to 0.7, p < 0.001). In that model, [log.sub.10], viral
load and episiotomy or perineal tear remain independent risk factors.
Table 4. Association between maternal viral load and placental malaria
among women who did and did not transmit HIV perinatally to their
infants, western Kenya, 1996-2001
Geometric mean HIV
viral load (a)
p value
Transmitters Nontransmitters (b)
All women (N = 455) 7,083 1,378 <0.001
Placental malaria-positive 41,217 1,675 <0.001
Placental malaria-negative 5,402 1,286 <0.001
p value 0.002 0.26
(a) Viral load expressed as copies per microliter of plasma.
(b) p from t test.
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Placental antigen-specific cytokine responses are impaired in human immunodeficiency virus-infected women. J Infect Dis 2000;182:960-4. (44.) Patterson BK, Behbahani H, Kabat WJ, Sullivan Y, O'Gorman MR, Landay A, et al. Leukemia inhibitory factor inhibits HIV-1 replication and is upregulated in placentae from nontransmitting women. J Clin Invest 2001;107:287-94. (45.) Berger EA, Murphy PM, Farber JM. Chemokine receptors as HIV-1 coreceptors: roles in viral entry, tropism tropism (trōp`ĭzəm), involuntary response of an organism, or part of an organism, involving orientation toward (positive tropism) or away from (negative tropism) one or more external stimuli. , and disease. Annu Rev Immunol 1999;17:657-700. (46.) Chaisavaneeyakorn S, Moore JM, Mirel L, Othoro C, Otieno J, Chaiyaroj SC, et al Levels of macrophage inflammatory protein 1 alpha (MIP-1 alpha) and MIP-1 beta in intervillous blood plasma samples from women with placental malaria and human immunodeficiency virus infection. Clin Diagn Lab Immunol 2003;10:631-6. (47.) WHO expert committee on malaria, twentieth report. Geneva: World Health Organization; 2000. (48.) van't Hoog AH, Otieno JA, Mature L, Obare-Okeyo R, Taren D, Misore A, et al. Low uptake of services in a pilot prevention of mother to child HIV transmission (PMCT PMCT Port Movement Control Team ) program in Kisumu, Western Kenya. XIV International AIDS Conference Education, networking and the promotion of best practice are essential to enhancing the response to HIV/AIDS. IAS conferences provide opportunities to share experience, and increase the knowledge and expertise of professionals working in HIV/AIDS. ; 2002 Jul 7-12; Barcelona, Spain. Abstract no. MoOrF1033. Dr. Ayisi is a senior research officer at the Centre for Vector Biology and Control Research, Kenya Medical Research Institute, Kisumu. His research interests include the epidemiology and control of malaria in pregnancy. Address for correspondence: Robert D. Newman, Malaria Branch, Centers for Disease Control and Prevention, 4770 Buford Highway NE, Mailstop F22, Atlanta, GA 30341, USA; fax: 770-488-4206; email: ren5@cdc.gov John G. Ayisi, * ([dagger]) Anna M. van Eijk,* ([dagger]) Robert D. Newman, ([double dagger]) Feiko O. ter Kuile, * ([dagger]) ([double dagger]) Ya Ping Shi, * ([double dagger]) Chunfu Yang, ([double dagger]) Margarette S. Kolczak, ([double dagger]) Juliana A. Otieno, ([section]) Ambrose O. Misore, ([section]) Piet A. Kager, ([dagger]) Renu B. Lal, ([double dagger]) Richard W. Steketee, ([double dagger]) and Bernard L. Nahlen ([double dagger]) ([paragraph]) * Centre for Vector Biology and Control Research, Kenya Medical Research Institute, Kisumu, Kenya; ([dagger]) University of Amsterdam, Amsterdam, The Netherlands; ([double dagger]) Centers for Disease Control and Prevention, Atlanta, Georgia, USA; ([section]) Ministry of Health, Kisumu, Kenya; and ([paragraph]) World Health Organization, Geneva, Switzerland |
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