Evaluation of in vivo antitrypanosomal activity of crude extracts of Artemisia abyssinica against aTrypanosoma congolense isolate.

BACKGROUND: African trypanosomiasis is a major disease of economic and public health importance affecting agricultural and human development. The search for alternative compounds against African trypanosomiasis is justified by various limitations of existing chemotherapeutic agents. This study was aimed at screening the hydromethanolic and dichloromethane (DCM) crude extracts of aerial parts of Artemisia abyssinica for in vivo antitrypanosomal activity against Trypanosoma congolense isolate in mice.
METHODS: The aerial parts of the plant were extracted by maceration technique using dichloromethane and 80% methanol to obtain the corresponding crude extracts. The plant extracts at doses of 100, 200 and 400 mg/kg body weight were administered intraperitoneally daily for 7 days to mice infected with Trypanosoma congolense. Diminazene aceturate and distilled water were used as positive and as negative controls respectively. The level of parasitaemia, body weight, packed cell volume, differential leukocyte counts and mean survival period were monitored.
RESULTS: The study showed that the DCM extract at 200 and 400 mg/kg, and the hydromethanolic extract at 400 mg/kg reduced parasitaemia (p < 0.05), ameliorated anaemia (p < 0.05), prevented body weight loss (p < 0.05) and resulted in significant increase in neutrophil levels (p < 0.05) and marked decrease in lymphocyte levels (p < 0.05) compared to the negative control.
CONCLUSIONS: This study established that aerial parts of A. abyssinica have antitrypanosomal potential and can be considered a potential source of new drugs for the treatment of tropical diseases caused by trypanosomes.

Background

African trypanosomiasis, a parasitic infection caused by single-celled protozoan parasites of the genus Trypanosoma that are primarily transmitted by the bite of infected tsetse flies. Human trypanosomiasis is caused by two sub-species of Trypanosoma brucei: T. brucei gambiense, and T. brucei rhodesiense while African animal trypanosomiasis is a group of diseases of ruminants, camels, equines, swine and carnivores caused by different trypanosome species [1-3]. Both, human and animal trypanosomiases negatively affect the whole economy of Africa by weakening both human and animals health [4].The unavailability of vaccine against trypanosomiasis and escalating costs of initiating and maintaining tsetse control campaigns have led to the vast tsetse infested areas of Africa being almost completely reliant on the use of trypanocidal drugs [5]. However, only a small group of chemoprophylactic and chemotherapeutic trypanocidal compounds are currently in use to which resistance has developed [6]. Furthermore, the registered trypanocides are beset with several additional drawbacks such as frequent toxicity, lengthy parenteral administration, lack of efficacy and unaffordable price [7]. The need for alternative new molecules that are safe, effective and affordable is urgent. It has been observed that natural products derived from plants offer novel possibilities to obtain new drugs that are active against trypanosomes and investigation of antitrypanosomal activity of traditionally used plants has been a major area of contemporary research focus [8]. In recent years, very small Ethiopian potential medicinal plants have been studied for their antitrypanosomal activity [9,10]. There is a need for the development of new agents to complement the existing drugs for the treatment of African trypanosomiasis. Artemisia abyssinica, known by various common names in Ethiopia, is used as a traditional remedy for several infectious and noninfectious diseases including typanosomiasis [11-13]. Nibret and Wink [9] reported the in vitro antitrypanosomal activity and cytotoxicity of the plant against drug sensitive T. brucei. Our former report [14] shows significant in vitro antitrypanosomal activity of crude extracts of aerial parts of the plant against T. congolense. Therefore, this study was aimed to evaluate the in vivo antitrypanosomal activity of crude extracts of aerial parts of the plant against field isolate of T. congolense in mice models of infection.

Methods

Chemicals

The chemicals and reagents used for the experiment include absolute methanol (Cheshire, UK), dichloromethane (ReAgent Chemical Services Ltd, UK), Tween-80 (BDH Laboratory supplies Ltd, England), phosphate buffered saline (PBS), 10% Giemsa stain (Shenyang Xin Guang, China), diminazene aceturate (Techno Pharmchem, India).

Plant material

Fresh aerial parts of A. abyssinica were collected in November 2011 from Sebeta, Oromia Regional State, about 24 km South of Addis Ababa, Ethiopia. The fresh plant material was wrapped with plastic sheets during transportation. The plant specimen was identified by a taxonomist in the Department of Biology and voucher specimen (TF001) was deposited at the National Herbarium, Addis Ababa University, Ethiopia.

Test organisms and experimental animals

The stocks of T. congolense that were originally isolated from a pure natural infection of cattle in Arba Minch, Ethiopia were obtained from the School of Veterinary Medicine, Addis Ababa University. The organisms were maintained by serial passages in mice until required as used and described by different workers [15,16]. Swiss albino mice (25–35 g) of both sexes aged 8–12 weeks, obtained from the breeding colony of the Akililu Lemma Institute of Pathobiology, Addis Ababa University, were used for conducting experiments. Protocols for this experiment were in accordance with the guidelines on care and wellbeing of research animals [17] and were approved by research and ethics committee of the School of Pharmacy, Addis Ababa University.

Preparation of plant extract

The collected plant material was shade dried at room temperature and crushed into powder using laboratory mortar and pestle. The powdered specimen was then extracted by maceration technique using dichloromethane and 80% methanol to obtain the corresponding crude extracts. Briefly, 100 g of the powdered plant material was weighed out and soaked separately in 1000 ml of solvents for 72 hours. The mixture was first filtered using gauze and then the filtrate was passed through sterile filter paper (Whatman No. 3, Whatman Ltd. England). Then the filtered extract was dried in an oven (hydromethanolic extract) at a temperature of 40°C and in rotary evaporator (dichloromethane extract) at 38.5-42°C. The resulting extract was then weighed, recorded and kept in a refrigerator until required for use.

Acute toxicity study

Acute toxicity study was done using the limit test dose of 2000 mg/kg according to OECD guideline for testing of chemicals using mice [18]. Six female Swiss albino mice separately received orally 2000 mg/kg of the hydromethanolic and DCM extracts. The mice were observed continuously for 1 h after administration of the extracts; intermittently for 4 h, over a period of 24 h and for 14 days for gross behavioral changes and other signs of toxicity manifestations. The acute toxicity study indicated that there were no visible signs of acute toxicity and death was not observed at the limit dose tested (2000 mg/kg) during the 14 days observation period.

Parasite inoculation and extract administration

The isolates were first inoculated heavily (104 trypanosomes/mouse) to donor mice. After establishment of infection (11–12 days post-inoculation), the donor mice were then subjected to cardiac puncture and blood was collected and immediately diluted with PBS for subsequent in vivo test. A total of sixty healthy mice were randomly grouped (n = 6) into ten groups (A-I, A-II, A-III, B-I, B-II, B-III, C, D, E and F). All experimental groups of mice (except group F) were then infected intraperitoneally with 2000 trypanosomes/mouse in 0.2 ml of blood as described and used by Ene et al. [19]. The animals were left to develop parasitaemia, and when average parasitaemia became approximately 107.03 parasites/ml, groups A-I, A-II and A-III were administered 100, 200 and 400 mg/kg of the hydromethanolic extract respectively. Whereas groups B-I, B-II and B-III received respectively 100, 200 and 400 mg/kg of the DCM extract. Dose of extracts were selected based on the results of acute toxicity. The extracts were administered to these groups intraperitonneally every morning for seven days. The extracts were dissolved and reconstituted in 2% Tween-80 in distilled water. Group C and D received 3.5 and 28 mg/kg (intraperitoneal single dose) of standard drug, diminazene aceturate, respectively. Group E consisted of the negative control which were infected with the parasite and received the vehicle. The group F included uninfected-untreated mice for reference.

Determination of parasitaemia and body weight change

The degree of parasitaemia was determined using the method of Herbert and Lumsden [20]. Briefly, the method involves microscopic counting of parasites per field in blood smears from the peripheral blood obtained from tail vein of of each mouse. Wet smears were prepared in triplicates from each animal and the mean value of slide counts was taken per sample examined microscopically. Logarithm values of these counts were obtained by matching with the table given by Herbert and Lumsden [20]. Parasitaemia was monitored every other day until the 14th day and twice a week thereafter.

For the assessment of antitrypanosomal effect of the extracts, the level of parasitaemia (expressed as log of absolute number of parasites per ml of blood) in the treated animals was compared to that of the control animals. The body weight of each mouse in all groups was also measured on the day treatment commenced (day 0) and every other day up to day 14 by a sensitive digital weighing balance.

Determination of packed cell volume and differential white blood cell count

The peripheral blood obtained from tail vein of of each mouse was used for determination of packed cell volume and differential white blood cell count. PCV was measured on days 0, 7 and 14 using Wintrobe’s method to predict the effectiveness of the test extracts in preventing haemolysis resulting from increasing parasitaemia associated with trypanosomiasis. The differential white blood cell (WBC) counts were determined on Giemsa-stained thin blood films obtained from each mouse on the 14th day of extract administration.

Determination of mean survival time

Mortality was monitored daily and the number of days from the time of inoculation of the parasite up to death was recorded for each mouse in the treatment and control groups throughout the follow up period for six weeks.

Statistical analysis

Values of the data obtained from the study were summarized and expressed as mean ± standard error of mean. Data analysis was performed using Statistical Packagefor Social Science (SPSS), version 16.0. To compare the results obtained from different groups, one way ANOVA followed by Tukey’s multiple comparison tests was performed to determine statistical significance. P values less than 0.05 were considered significant.

Results

Effect of crude extracts on parasitaemia

There were fluctuations in the level of parasitaemia of all the treated groups which were, however, kept at relatively low or very low level relative to infected-untreated control especially at higher doses of both extracts. The best results were obtained with DCM extract at an optimum dose of 400 mg/kg (Table 1) which was less effective compared with 28 mg/kg of standard drug. Comparison with the negative control revealed that the 400 mg/kg DCM extract has kept parasitaemia at a significantly low level (p < 0.05 on days 4 through 14) and 200 mg/kg had considerably reduced parasitaemia (p < 0.05) on days 6 and 8 of treatment. The mice treated with 400 mg/kg hydromethanolic crude extract had significantly reduced parasitaemia (p < 0.05 on days 6, 8 and 10 of treatment) when compared with the infected-untreated group. Maximum dose (28 mg/kg) of the standard (DA) was able to temporarily clear the parasites from circulation within two days of treatment although parasites reappeared from day 12 of treatment until all animals relapsed on day 16.83 ± 1.28 (Tables 1 and 2). The 3.5 mg/kg DA was not able to even briefly clear the trypanosomes from all animals right from the beginning and relapse in this group was recorded in all animals after day 6.16 ± 1.42 of treatment. Comparison between the groups treated with the two types of extracts indicated that the DCM extract appeared to be superior to the hydromethanolic extract in reducing the parasite burden. The results showed that mice treated with 400 mg/kg of DCM extract had continually reduced parasitaemia level from day 2 of treatment to day 8 which was further kept on average at lowest level up to the end of the monitoring period. However, parasitaemia reduction at higher doses, 400 and 200 mg/kg, of DCM extract and 400 mg/kg hydromethanolic extract were not significantly different.

Table 1

Effect of dichloromethane crude extract of aerial parts of on parasitaemia and mean survival time of infected mice

Treatment	Dose (mg/kg)	Parasitaemia level (log number)/ml								Mean survival time (days)
		D0	D2	D4	D6	D8	D10	D12	D14
DCM ext	100	6.68 ± 0.23	7.08 ± 0.25	7.57 ± 0.26bc	7.83 ± 0.14bcd	6.31 ± 0.46cd	6.70 ± 1.37c	7.31 ± 0.44cd	6.41 ± 1.34c	34.33 ± 4.63
DCM ext	200	7.05 ± 0.18	7.04 ± 0.23	5.65 ± 1.18bc	3.80 ± 1.20a	3.92 ± 1.37a	6.70 ± 0.30c	6.78 ± 0.39c	7.07 ± 0.32c	37.83 ± 3.49
DCM ext	400	7.00 ± 0.30	6.95 ± 0.26	4.90 ± 0.98ac	2.80 ± 1.26a	1.95 ± 1.24a	3.70 ± 1.17a	4.85 ± 0.99abc	4.95 ± 1.01a	40.67 ± 2.42
DA	3.5	7.09 ± 0.06	1.25 ± 1.25	1.90 ± 1.20a	3.30 ± 1.48a	4.60 ± 1.48c	6.12 ± 1.26c	7.41 ± 0.40cd	7.92 ± 0.27c	36.83 ± 4.36
DA	28	7.13 ± 0.05	0.00 ± 0.00	0.00 ± 0.00a	0.00 ± 0.00a	0.00 ± 0.00ab	0.00 ± 0.00f	0.90 ± 0.90e	1.85 ± 1.17f	42.00 ± 0.00
Distilled water	1 ml	6.94 ± 0.26	7.97 ± 0.12	8.67 ± 0.10	8.54 ± 0.07	8.46 ± 0.17	8.70 ± 0.06	8.14 ± 0.27	8.45 ± 0.21	34.33 ± 6.15

Values are mean ± SEM; n = 6; D = day; D0 = the day treatment commenced; SEM = standard error of mean; DCM = Dichloromethane; ext = extract; DA = Diminazene aceturate; All superscripts indicate significance at p < 0.05 (a = compared to negative control; b = compared to 3.5 mg/kg DA; c = compared to 28 mg/kg DA; d = compared to 400 mg/kg; e = compared to all groups, f = compared to all groups but 400 mg/kg).

Table 2

Effect of hydromethanolic crude extract of aerial parts of on parasitaemia and mean survival time of infected mice

Treatment	Dose (mg/kg)	Parasitaemia level (log number)/ml								Mean survival time (days)
		D0	D2	D4	D6	D8	D10	D12	D14
80% MeOH ext	100	7.16 ± 0.18	8.10 ± 0.17	7.80 ± 0.28bc	7.92 ± 0.26bcd	7.88 ± 0.16c	8.23 ± 0.21c	7.82 ± 0.16c	8.45 ± 0.13c	35.17 ± 6.49
80% MeOH ext	200	7.02 ± 0.09	7.90 ± 0.08	7.57 ± 0.24bc	6.90 ± 0.49c	6.70 ± 0.47c	7.95 ± 0.24c	7.69 ± 0.33c	8.10 ± 0.27c	36.50 ± 5.09
80% MeOH ext	400	7.17 ± 0.32	7.83 ± 0.28	6.05 ± 0.36bc	3.00 ± 1.36a	3.87 ± 1.37a	4.90 ± 1.00ac	7.30 ± 0.12c	7.15 ± 0.31c	38.17 ± 4.88
DA	3.5	7.09 ± 0.06	1.25 ± 1.25	1.90 ± 1.20ad	3.30 ± 1.48a	4.60 ± 1.48c	6.12 ± 1.26c	7.41 ± 0.40c	7.92 ± 0.27c	36.83 ± 4.36
DA	28	7.13 ± 0.05	0.00 ± 0.00	0.00 ± 0.00ad	0.00 ± 0.00a	0.00 ± 0.00ab	0.00 ± 0.00e	0.90 ± 0.90e	1.85 ± 1.17e	42.00 ± 0.00
Distilled water	1 ml	6.94 ± 0.26	7.97 ± 0.12	8.67 ± 0.10	8.54 ± 0.07	8.46 ± 0.17	8.70 ± 0.06	8.14 ± 0.27	8.45 ± 0.21	34.33 ± 6.15

Values are mean ± SEM; n = 6; D = day; D0 = the day treatment commenced; SEM = standard error of mean; MeOH = Methanol; ext = extract; DA = Diminazene aceturate; All superscripts indicate significance at p < 0.05 (a = compared to negative control; b = compared to 3.5 mg/kg DA; c = compared to 28 mg/kg DA; d = compared to 400 mg/kg; e = compared to all groups).

Effect of crude extracts on body weight

Treatment with the crude extracts prevented loss of weight associated with parasitaemia particularly at 200 and 400 mg/kg dose levels of DCM extract and with 400 mg/kg of hydromethanolic extract compared to the negative controls. There were no detectable differences in preventing weight loss associated with parasitaemia between the extracts as well as between the extracts and standard (3.5 mg/kg) at these dose levels throughout the monitoring period (Figure 1a and b). Considerable body weight improvement was seen by 28 mg/kg DA (12.9%) followed by 400 mg/kg DCM extract (11.42%) relative to the pre-treatment value.

Figure 1

Effect of extract of on body weight of mice. (a) hydromethanolic crude extract (b) dichloromethane crude extract. Values are mean ± SEM; n = 6; D = day; D0 = the day treatment commenced; a = p < 0.05 compared to negative control; b = p < 0.05 compared to 28 mg/kg DA.

Effect of crude extracts on packed cell volume

As shown in Figure 2, administration of the plant extracts to the infected group produced a substantial difference in PCV when compared with the infected-untreated group. The prevention of PCV reduction observed at 200 mg/kg and 400 mg/kg DCM extracts over the infected-untreated group was comparable. These values were also comparable between these dose levels and to that caused by the standard at 28 mg/kg with no statistically significant difference.

Figure 2

Percentage packed cell volume change of infected mice treated with hydromethanolic and dichloromethane crude extracts of aerial parts of Values are mean ± SEM; n = 6; PCV = packed cell volume; A = Hydromethanolic extract; B = Dichloromethane extract; I = 100 mg/kg; II = 200 mg/kg; III = 400 mg/kg; C = 3.5 mg/kg DA; D = 28 mg/kg DA; E = Negative control; F = uninfected-untreated.

Effect of crude extracts on differential white blood cell count

The results in Figure 3a and b indicate that differential white blood cell (WBC) count revealed that% lymphocyte counts were significantly higher (p < 0.05) in the groups that received lowest dose (100 mg/kg) of both extracts, 3.5 mg/kg DA and in the infected-untreated group compared to uninfected-untreated group; whereas marked decrease (p < 0.05) in neutrophil count was noticed in these groups.

Figure 3

Effect of extract of on differential white blood cell count of mice. (a) hydromethanolic crude extract (b) dichloromethane crude extract. Values are mean ± SEM; n = 6; UU = uninfected-untreated; WBC = white blood cell; a = p < 0.05 compared to negative control; b = p < 0.05 compared to uninfected-untreated.

The lymphocyte and neutrophil levels in the remaining experimental groups were comparable to that in the uninfected-untreated group. Comparison with the negative control, neutrophil levels in all treated groups except 100 mg/kg hydromethanolic extract, showed noticeable increase (p < 0.05) while lymphocyte levels showed marked decrease (p < 0.05) except in those groups that received lowest dose (100 mg/kg) of both extracts and 3.5 mg/kg DA in which the values were similar.

Effect of crude extracts on mean survival time

Analysis of the mean survival time (days) revealed that only all the mice treated with DA (28 mg/kg) survived throughout the period of the study (42.00 ± 0.00) compared to groups that received the extracts, standard dose of DA (3.5 mg/kg) and the infected-untreated control. Among the extract treated animals, the group treated with DCM extract at 400 mg/kg had the highest mean survival time of 40.67 ± 1.00 days (Tables 1 and 2).

Discussion

The objective of the present study was to evaluate the in vivo antitrypanosomal activity of crude methanolic and dichloromethane extracts of aerial parts of A. abyssinica against field isolate of T. congolense in mice models of infection. The in vivo mice study revealed that the extracts did not completely eliminate the trypanosomes from the blood stream of infected mice, but considerably reduced level of parasitaemia. Though parasitaemia was not completely eliminated, taken as a whole, the DCM extract had the highest antitrypanosomal activity compared to the hydromethanolic extract and the untreated control. Several other workers also made similar observation on the differentially high antitrypanosomal activity produced by lipophilic extracts (DCM, chloroform, petroleum ether) of different plants both in vivo and in vitro (10, 15,19). The finding is in agreement with our former report which showed that DCM extract had better in vitro antitrypanosomal activity than hydromethanolic extract [14].

The hydromethanolic extract similarly reduced parasitaemia but only at its optimum dose of 400 mg/kg body weight. The high parasite load attained before commencement of treatment, enzymatic inactivation of active compounds and impaired absorption from the site of administration could mask efficacy of crude extracts to completely clear the parasites in the blood [21-23]. The fact that the plant showed differential activity between extracts is confirmation of earlier assertions [24] that any statement on a plant’s trypanocidal activity should be taken within the context of the plant part and the solvent extract tested. This is because difference in solvent of extraction may reveal different phytochemicals in the same plant. A similar finding to earlier reports [15,19,24] in the difference in composition of secondary metabolites was observed with the two solvents of extraction in this investigation which could in part contribute to the activity difference.

Although diminazene aceturate was able to temporarily clear trypanosomes from circulation of infected mice, relapse occurred in all experimental mice approximately on days 6 and 16 of treatment respectively at 3.5 and 28 mg/kg dose levels. This observation was not surprising as trypanocidal drug resistance has been wide spread in several African countries including Ethiopia [25-28].

The present study did not involve detailed characterization and isolation of different compounds that could be responsible for the observed activity. However, phytochemical screening revealed the presence of tannins, flavonoids, alkaloids, cardiac glycosides and polyphenols in the hydromethanolic extract, and terpenoids, polyphenols and phytosteroids in the DCM extract [14].

The antitrypanosomal effect shown by extracts in this study might be attributed to the presence of one or more of these constituents which, in contrast to synthetic pharmaceuticals based upon single chemicals, may exert their effects through the additive or synergistic action of several chemical compounds acting at a single or multiple target sites associated with a physiological process [29].

Several possible mechanisms working separately or in concert may account for the observed effect [30]. Accumulated evidences suggest that many natural products exhibit their antitrypanosomal activity by virtue of their interference with the redox balance of the parasites acting either on the respiratory chain or on the cellular defenses against oxidative stress [24]. This is because natural products possess structures capable of generating radicals that may cause peroxidative damage to trypanothione reductase that is very sensitive to alterations in redox balance. Published reports also indicate that several natural products such as alkaloids, polyphenols, terpenoids and saponins that primarily interact with important molecular targets such as DNA, microtubules, biomembranes, receptors and may induce cytotoxicity and death in trypanosomes. Several active alkaloids are known to intercalate DNA, and in consequence inhibit DNA and RNA polymerase, topoisomerases, ribosomal protein biosynthesis, or bind to tubulin/microtubules, thus acting as spindle poisons to disturb membrane integrity in trypanosomes [31].

Trypanosome generated reactive oxygen species can also attack red blood cells’ membranes, induce oxidation and subsequently hemolysis. Thus, scavenging the trypanosome associated free radicals by phytochemicals such as flavonoids and other polyphenolic antioxidants may ameliorate anemia induced by trypanosome infection [32]. The plant extracts may strengthen the host defense that was already activated because of the presence of trypanosomes in circulation with established infection [33].

The mechanism by which these extracts exhibited their antitrypanosomal activity can only be speculated since the active ingredient(s) were not isolated. Several investigations tend to suggest that it is often difficult to speculate and decipher the exact mode of action by which plant extracts exhibit their trypanocidal action. Indeed, the possible mechanisms by which plant extracts and phytochemicals therein carry out this role remain a subject of great speculations and debate in the scientific community [34]. Thus, for the DCM extract in our study, the antitrypanosomal effect produced would most likely be ascribed to either of the terpenoids, polyphenols or phytosteroids detected in the extract. However, rare findings have suggested as to how any of these phytochemicals produce their antitrypanosomal activity. The result of Nibret et al.[10] has clearly indicated that out of the 40 plant extracts tested, the DCM extract from stem bark of Warburgia salutaris (claimed to be used against many pathologies in many parts of Africa) was found to exhibit the most potent trypanocidal activity. The trypanocidal activity was suggested to be due to the drimane sesquiterpenoids (warburganal and polygodial). Concerning the mechanism, it was proposed that the two sesquiterpene aldehydes, warburganal and polygodial, formed covalent bonds with amino groups of proteins and affect a vast number of cellular activities.

The positive effect of the extracts against trypanosome infection can further be deduced from the weight status of the animals and the body weight improvement was consistent with the observation made on parasitaemia. This observation indicates that the animals with better physical state could feed more than those in the other groups and resist weight loss that is usually associated with trypanosomiasis.

The observed antitrypanosomal effect of the extracts in this study was accompanied by corresponding improvement and prevention of further drop in PCV suggesting that they have potentials to ameliorate anaemia. This could possibly be by reducing the proliferating parasite load, neutralizing the toxic metabolites produced by trypanosomes or scavenging the trypanosome associated free radicals [15,21,35]. This was particularly noticed in the second week of treatment, in groups with significantly reduced parasitaemia, where the final PCV values were almost similar to the pre-treatment values. The infected mice treated with the standard drug (diminazine aceturate) at 28 mg/kg showed nearly stable PCV up to day 14 of treatment although relapse occurred in all animals after 16 days post treatment. In contrast, the recommended standard dose for cattle and mice (3.5 mg/kg) was unable to prevent PCV reduction suggesting its failure to eliminate parasitaemia. Similar observations have been reported in previous studies [26,36,37].

Lymphocytes are the main effector cells of the immune system [38]. Results of the differential white blood cell count revealed that higher differential lymphocyte counts were generally recorded in those groups in which parasitaemia was not relatively kept in check and in the infected-untreated. Leucocytosis which may be due to lymphocytosis have been implicated in trypanosomiasis and these conditions are usually as a result of wax and wear syndrome on the animal immune system caused by the ever changing variable surface glycoprotein of the infecting trypanosomes [39] that demands the immune system to continuously produce antibodies and hence keep the level of lymphocytes high. However, administration of the extracts that have significantly lowered parasitaemia seemed to prevent lymphocytosis suggesting that this phenomenon is a result of parasite load. Hence, the relatively reduced percentage of lymphocytes post extract treatment suggests that the plant extracts by suppressing parasitaemia contributed to the attenuation of the immunological reaction.

The lower differential counts of neutrophils observed in the infected negative control and groups in which parasitaemia was persistently higher may be attributed to the immunosuppressive actions of trypanosome infection [39-41]. Several mechanisms such as granulocyte hypoplasia and splenic sequestration have been proposed for neutropenia in African trypanosomiasis [42]. It has been suggested that granulocyte progenitor cells may be coated with trypanosome antigen-antibody as occurs with RBC leading to phagocytosis [43]. In this study, we suggest that treatment with crude extracts of aerial parts A. abyssinica has reduced parasite load consequently leading to a decrease in coating of the progenitor cells which prevented or reduced the development of neutropenia.

Neither the extracts nor the standard drug cured the infection although parasitaemia was kept in check. Earlier reports indicated that in T. congolense infections probably the long lasting chronic wasting situation and a complex process of gradual impairment of organs and tissues of the host lead to the eventual generalized collapse. A sufficiently balanced situation in the host-parasite relationship might allow the establishment of a chronic infection that could lead to survival of infected animals for several months [44]. The mice in all groups that showed high levels of parasitaemia survived for at least 34 days showing that they resisted the parasites for appreciable period of time.

Conclusion

In vivo assay of the present investigation has provided evidence that extracts of aerial parts of A. abyssinica have reduced parasite burden and ameliorated anaemia, prevented body weight loss, increased neutrophil levels and decreased lymphocyte levels as a consequence of the parasites being kept in check and DCM extract showed a superior antitrypanosomal activity than hydromethanolic extract. This study established that aerial parts of A. abyssinica have antitrypanosomal potential and can be considered a potential source of new drugs for the treatment of tropical diseases caused by trypanosomes.

Abbreviations

DCM: Dichloromethane; DA: Diminazine aceturate; T.congolense: Trypanosoma concolense; A. abyssinica: Artemisia abyssinica; PCV: Packed cell volume; WBC: White blood cell.

Competing interests

The authors declare that they have no competing interests.

Authors’ contributions

TF conceived the study, designed and conducted all laboratory experiments; analysed and interpreted experimental results. WS and GT participated in the proposal, study design and manuscript preparations. All authors read and approved the final manuscript.

Pre-publication history

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http://www.biomedcentral.com/1472-6882/14/117/prepub