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Original Research

Hematological abnormalities in HIV-antiretroviral therapy naïve clients as seen at an immune suppression syndrome clinic at Mbarara Regional Referral Hospital, southwestern Uganda

Crispus Katemba1 Department of Medical Laboratory Sciences, Mbarara University of Science and Technology, Mbarara, Uganda
,
Conrad Muzoora2 Department of Internal Medicine, Mbarara University of Science and Technology, Mbarara, Uganda
,
Enoch Muwanguzi1 Department of Medical Laboratory Sciences, Mbarara University of Science and Technology, Mbarara, Uganda
,
Bashir Mwambi3 Institute of Allied Health Sciences, Clarke International University, Kampala, Uganda, [email protected]
,
Christine Atuhairwe4 Institute of Public Health and Management, Clarke International University, Kampala, Uganda
&
Ivan M Taremwa3 Institute of Allied Health Sciences, Clarke International University, Kampala, Uganda, [email protected]Correspondence[email protected]
Pages 105-110 | Published online: 27 Jun 2018

Abstract

Aim/objective

To assess the common hematological abnormalities among HIV-antiretroviral therapy (ART) naïve clients attending an immune suppression syndrome (ISS) clinic at Mbarara Regional Referral Hospital (MRRH), southwestern Uganda.

Patients and methods

This was a cross-sectional study carried out during the months of March to August 2016 at the ISS clinic of MRRH. We collected approximately 4.0 mL of EDTA anticoagulated blood samples, which were assayed for complete blood count, CD4+ cell count and thin film examination. Correlation of the hematological abnormalities with CD4+ cell counts was done using correlation coefficient (r) and analysis of variance (F), and the p-value was set at ≤0.05.

Results

A total of 141 clients were enrolled. Of these, 67.38% (95/141) were anemic, 26.24% (40/141) had thrombocytopenia while 26.95% (38/141) had leucopenia. Of the 95 participants with anemia, 89.47% (85/95) presented with normocytic-normochromic anemia, 8.42% (8/95) with microcytic-hypochromic anemia and 2.11% (2/95) with macrocytic-hypochromic anemia. Anemia was not different across the several World Health Organization (WHO) stages of HIV infection disease progression (p>0.05). Statistically significant differences were present among participants with leucopenia (p<0.05). Also, leucopenia was more prevalent (11/38) among participants in WHO stage 4 of HIV infection. CD4+ cell counts correlated with thrombocytopenia (r=0.24, p<0.05) and leucopenia (r=0.15, p<0.05).

Conclusion

People living with HIV/AIDS (PLWHIV/AIDS) ought to be routinely monitored and treated for the occurrence of hematological abnormalities. Early initiation of ART can help to prevent some hematological abnormalities.

Introduction

According to the Uganda AIDS Commission (UAC), HIV remains a threat, as evidenced by the prevalence rate increasing from 6.4% to 7.3%.Citation1 Consequently, some of the HIV-infected individual will progress to the AIDS state, which is a systemic disorder characterized by severe impairment and progressive damage of both cellular and humoral immune responses. Over time, hematological abnormalities have been documented as independent predictors of morbidity and mortality among HIV-infected individuals.Citation2,Citation3 As part of routine monitoring and diagnosis, the use of cluster of differentiation (CD), especially CD4-T lymphocyte marker and full blood count, has been vital as pre-treatment investigations for people living with HIV/AIDS (PLWHIV/AIDS).Citation4,Citation5 This has demonstrated changes in blood cells, which are indicative of the effect of HIV infection.Citation5 Although they are neither part of the criteria for initiating therapy, nor used by the World Health Organization (WHO) for staging HIV, hematological abnormalities indicated by deranged full blood count are common manifestations and important prognostic tools of HIV infection and AIDS.Citation6 Anemia, leucopenia and thrombocytopenia are common during the course of HIV infection, and may be due to the direct effects of HIV infection, secondary infections or side effects of anti-retroviral therapy.Citation7

Cytopenias are common in the advanced stages of AIDS and often caused by concomitant myelosuppressive drugs. Although hematological abnormalities are common in HIV infected clients and have great effect on their well-being and treatment, few studies on this have been undertaken in Uganda. Thus, we report on the prevalence and pattern of hematological abnormalities in HIV antiretroviral therapy (ART) naïve clients at an immune suppression syndrome (ISS) clinic of Mbarara Regional Referral Hospital (MRRH), southwestern Uganda.

Patients and methods

Study participants

The participants were HIV sero-positive clients enrolled in the ISS clinic, MRRH, located within Mbarara Municipality, Mbarara district in southwestern Uganda.

Sample collection

Approximately 4 mL of blood was drawn by venipuncture from study participants into an EDTA vacutainer.

Laboratory analysis

Full blood count and CD4+ cell counts were done using the Coulter ACT 5Diff CP and Facscalibur, as per standard operating procedures at the ISS clinic. Reference ranges as determined for the HIV population were used.Citation8 Thrombocytopenia was regarded as platelet count less than 150×109/L, anemia was defined as hemoglobin concentration less than 12 g/L for adult females and less than 13 g/dL for adult males, and leucopenia was considered as white blood cell (WBC) count less than 2.75×109/L. Thin blood films were prepared, stained by Giemsa and examined for anemia typing based on: a) size of red blood cells (normocytic, microcytic and macrocytic) and b) hemoglobin content (normochromic and hypochromic). Pancytopenia was considered if all the three blood cells were below their minimum for a reference range. We ensured strict adherence to the standard operating procedures, the hematology analyzer was well maintained and controls were run daily before use. A hematology bench aid was used to ascertain cell features of a comprehensive film comment.

Statistical analysis

Descriptive statistics (mean, median, inter-quartile range and standard deviation) were used. The chi-square test, analysis of variance and Z tests were used to establish predictor variables. Proportions and percentages were calculated for categorical variables, and were compared using 95% confidence interval. Correlation of the hematological abnormalities with CD4+ cell counts was done using correlation coefficient (r) and analysis of variance (F). The p-value was set at ≤0.05.

Ethical considerations

We obtained ethical approval from Mbarara University of Science and Technology Faculty of Medicine Research and Ethics Committee (FREC), and the university’s Research and Ethics Committee (REC). All participants provided written informed consent.

Results

A total of 141 HIV positive ART naïve participants were enrolled. This was a cohort of advanced HIV disease with the overwhelming majority of participants with CD4 cells below 350. They comprised 56.03% (n=79) males. Their mean age was 34 years (95% CI=33, 36 years); the minimum and maximum age was 17 and 63 years respectively, with a median age of 32 years (interquartile range [IQR] 28, 42 years). Their socio-demographic, hematological and immunologic features are presented in .

Table 1 Demographic, hematologic and immunologic characteristics of study participants (n=141)

Of the 141 participants, 67.38% (95% CI=58.98–75.03) were anemic, 26.24% (95% CI=19.19–34.31) had thrombocytopenia while 26.95% (95% CI=19.83–35.07) had leucopenia. The pattern of cytopenias was as follows: 62 (43.97%; 95% CI=40.54–58.68) had anemia alone, 17 (12.06%; 95% CI=8.13–20.88) had both anemia and thrombocytopenia while 11 (7.80%; 95% CI=4.48–15.2) had both anemia and leucopenia. Eight (5.67%; 95% CI=2.80–12.22) had thrombocytopenia alone, 7 (4.96%; 95% CI=2.28–11.19) had both thrombocytopenia and leucopenia while 15 (10.64%; 95% CI=6.87–19.02) had leucopenia alone. There were 5 (3.54%; 95% CI=1.31–9.09) participants who had pancytopenia.

Thin film examination showed most participants to have normocytic-normochromic anemia (85/95; 89.47%), then microcytic-hypochromic anemia (8/95; 8.42%) and least had macrocytic-hypochromic anemia (2/95; 2.11%). Microcytic-hypochromic anemia was more likely to occur (8/10; 80%) compared to normocytic-normochromic anemia (85/122; 69.67%) and macrocytic-hypochromic anemia (2/9; 22.22%) (χ2=9.37, p=0.009). Leucopenia was more associated with neutropenia (χ2=37.14; p<0.001) compared to lymphopenia (χ2=18.44; p<0.001). For platelet counts, 86.49%, (95% CI=71.23–95.46) had mild thrombocytopenia, while 3.51% (95% CI=4.54–28.74) had severe thrombocytopenia, as indicated in .

Table 2 Distribution of cytopenias (n=125)

WHO clinical staging indicated no difference in the prevalence of anemia and thrombocytopenia among all the clinical stages (Z=−1.23, p=0.22 and Z=2.74, p=0.06 respectively). Leucopenia was more among participants in clinical stage 4 (Z=2.08, p=0.03). The details are shown in .

Table 3 Hematological abnormalities at each WHO HIV stage

Correlation of the common hematological abnormalities with CD4+ cell counts showed that diminished CD4+ cell counts had no association with anemia (r=−0.0002), but the association exists with thrombocytopenia and leucopenia (r=0.24, and 0.15 respectively) as given in .

Table 4 Correlation of hematological abnormalities with CD4+ cell count

Discussion

Cytopenias have been widely reported among people living with HIV/AIDS.

Anemia was the most prevalent cytopenia, accounting for 67.38% (95% CI=58.98–75.03). This is similar to the 64.2% reported in India,Citation9 although lower than the 82.4% in a review.Citation10 The high prevalence is explained by the effect of myelodyplasia on the erythroid cells.Citation9,Citation11Citation13

Morphological characterization of anemia based on comprehensive film comment indicated normocytic-normochromic (85/95; 89.47%), microcytic-hypochromic (8/95; 8.42%) and macrocytic-hypochromic (2/95; 2.11%) types. Normocytic-normochromic anemia suggested continued bone marrow myelodyplasia.Citation9,Citation11 This occurs as a result of decreased ability of bone marrow to synthesize and release blood cells into circulation, a phenomenon that is evident in HIV infection, as well anti-retroviral therapy.Citation11 On the other hand, the variant (microcytic-hypochromic and macrocytic hypochromic) forms of anemia are nutrient deficiency indicators.Citation14Citation17 Nutrient deficiencies are common in clients with HIV immunosuppression, mainly due to the impact of anorexia, medication associated gastrointestinal disturbances, wasting and malabsorption.Citation17 In some cases, iron deficiency anemia secondary to HIV, related to gastrointestinal blood loss has been reported.Citation15Citation17 This is the probable explanation for the occurrence of microcytosis in our study. The etiology of vitamin B12 deficiency in these patients has been linked to malabsorption in the distal ileum and an alteration in cobalamin transport proteins.Citation14 Folate deficiency can occur in HIV-infected patients and may result from reductions in both dietary intake and intestinal absorption,Citation14 which explains the occurrence of macrocytic anemia among our study participants.

Thrombocytopenia accounted for 26.24% (95% CI=19.19–34.31). This was similar to what was found in Chinese adults.Citation18 On the other hand, results from this study were higher than the values of 8.3% and 17.8% reported in Uganda,Citation19,Citation20 and 5.9% in Ethiopia.Citation2 The pathogenesis of thrombocytopenia has been associated with immune causes,Citation18,Citation20,Citation21 which arise early in the course of HIV infection but are slightly more prevalent in those with advanced disease.Citation21

In this study, 26.95% (95% CI=19.83–0.07%) of the participants had leucopenia, results similar to the values of 26.8% and 26.6% found in Nigeria.Citation5,Citation22 In this study, leucopenia was more associated with neutropenia (χ2=37.14; p<0.001). This phenomenon is ascribed to the autoimmune destruction as the pathogenesis of neutropenia. In addition, HIV is a likely mediator of defective hematopoiesis through mechanisms like direct infection of early hemopoetic precursors, aberrations of local cytokine and growth factor signaling and changes in the bone marrow stroma.Citation3 As there is limited literature about demographic indicators of neutropenia, we attribute leucopenia to be the likely cause of neutropenia, as reported earlier.Citation3 Pancytopenia was seen in 3.54%, and this is attributed to opportunistic infections including Mycobacteria and fungi (including Pneumocystis carinii, Crypococcus neformas and Penicillium marneffei) that are capable of broad dissemination throughout the bone marrow, directly affecting the progenitor cells.Citation3

There was no difference in the prevalence of anemia and thrombocytopenia among all the WHO HIV clinical stages, but a difference occurred within the WBC population. Leucopenia was more common among participants in clinical stage 4 (Z=2.08, p=0.03). The fact that HIV affects the CD4+ and natural killer cells which are part of the population of WBCs can explain why we found leucopenia more in the advanced clinical stages (Z=2.08, p=0.03).Citation9,Citation11,Citation23

A correlation of the common hematological abnormalities with CD4+ cell counts indicated that deteriorating immune status had no statistical association with anemia (r=−0.0002), which was similar to other studies.Citation24Citation26 Besides immunological exposures, there are other causes of anemia in HIV infection, e.g. autoimmune antibodies to hemopoetic precursors and opportunistic infections like parvovirus B19, cytomegalovirus (CMV), or Mycobacterium aviumintracellulare which suppress erythropoiesis. Also hemolytic anemia, gastrointestinal bleeding and malnutrition with folate, vitamin B12 and iron have been reported to cause anemia in HIV infection.Citation27

A slight association exists with thrombocytopenia and leucopenia (r=0.24 and 0.15, respectively) to decreasing CD4+ cell counts. This was similar to results from Ethiopia.Citation2 As already elucidated, thrombocytopenia is associated with advanced AIDS.Citation20 Since CD4+ cell count is used as a feature of deteriorating HIV infection, this may explain the correlation between thrombocytopenia and lower CD4+ cell counts. Thus, there is a need to prevent CD4+ cell counts decreasing, which is achieved by early initiation of ART, and routine monitoring of the effectiveness of the different regimen.

The results of this study should be interpreted with the following limitations in mind: a) we did not investigate the risk of cytopenia due to opportunistic infections, yet this population was highly susceptible; b) we did not investigate the possibility of hemoglobinopathies as likely causes of anemia; c) although we attribute nutrient deficiency as a probable cause of nutritional anemia, we did not assay for iron, vitamin B12 and folate and d) we did not study the bone marrow, thus we are lacking the bone marrow hemopoetic picture.

Conclusion

We report a high risk of cytopenias (anemia, leucopenia and thrombocytopenia) among PLWHIV. The study has also found that a decrease in the CD4+ cell counts had no association with anemia, but an association exists with thrombocytopenia and leucopenia. Also, the occurrence of anemia and thrombocytopenia was not associated with any clinical stage, but those in clinical stage 4 were more likely to have leucopenia. With the high risk of cytopenias, it is imperative to initiate PLWHIV/AIDS on ART early, and routinely monitoring the response.

Author contributions

CK, IMT, CA, EM, CM and BM participated in study conception and design, data acquisition, analysis and interpretation, manuscript drafting and revising. CA, BM and IMT critically revised the manuscript. All authors read and approved the final manuscript and agreed to be accountable for all aspects of the work.

Acknowledgments

The authors would like to thank the study participants and the staff of ISS clinic.

Disclosure

The authors report no conflicts of interest in this work.

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