- Research Article
- Open Access
Efficacy of PermaNet® 3.0 and PermaNet® 2.0 nets against laboratory-reared and wild Anopheles gambiae sensu lato populations in northern Tanzania
Infectious Diseases of Poverty volume 6, Article number: 11 (2017)
Mosquitoes have developed resistance against pyrethroids, the only class of insecticides approved for use on long-lasting insecticidal nets (LLINs). The present study sought to evaluate the efficacy of the pyrethroid synergist PermaNet® 3.0 LLIN versus the pyrethroid-only PermaNet® 2.0 LLIN, in an East African hut design in Lower Moshi, northern Tanzania. In this setting, resistance to pyrethroid insecticides has been identified in Anopheles gambiae mosquitoes.
Standard World Health Organization bioefficacy evaluations were conducted in both laboratory and experimental huts. Experimental hut evaluations were conducted in an area where there was presence of a population of highly pyrethroid-resistant An. arabiensis mosquitoes. All nets used were subjected to cone bioassays and then to experimental hut trials. Mosquito mortality, blood-feeding inhibition and personal protection rate were compared between untreated nets, unwashed LLINs and LLINs that were washed 20 times.
Both washed and unwashed PermaNet® 2.0 and PermaNet® 3.0 LLINs had knockdown and mortality rates of 100% against a susceptible strain of An. gambiae sensu stricto. The adjusted mortality rate of the wild mosquito population after use of the unwashed PermaNet® 3.0 and PermaNet® 2.0 nets was found to be higher than after use of the washed PermaNet® 2.0 and PermaNet® 3.0 nets.
Given the increasing incidence of pyrethroid resistance in An. gambiae mosquitoes in Tanzania, we recommend that consideration is given to its distribution in areas with pyrethroid-resistant malaria vectors within the framework of a national insecticide-resistance management plan.
Please see Additional file 1 for translations of the abstract into the five official working languages of the United Nations.
For the past three decades, significant progress in malaria control has been largely attributed to the widespread use of insecticide-based vector control interventions including indoor residual spraying (IRS) and long-lasting insecticidal nets (LLINs) [1–5]. A LLIN is a factory-treated mosquito net that is expected to retain its biological activity for a standard number of washes and a for a period of not less than 3 years but not more than 5 years . Currently, a LLIN would be expected to retain its biological activity for at least 20 standard washes under laboratory conditions and 3 years of recommended use under field conditions, as defined in the recently-updated World Health Organization (WHO) guidelines .
The increasingly insecticide-resistant population of Anopheles gambiae sensu lato mosquitoes (hereafter referred to as An. gambiae) across Africa could represent a threat to the tools currently used for vector control [8–14]. Resistance to every currently used insecticide has been found and many factors are believed to increase vector resistance including the extensive use and misuse of the same classes of insecticides in agriculture and public health sectors .
Combined insecticides have reduced the level of resistance in the vector population , and rotating insecticides periodically has shown to be effective against wild vector populations or in delaying the build-up of insecticides resistance among vectors [11, 15, 16]. However, none of these options are able to reduce the metabolic activity of the mosquito against insecticides. Discovering a tool that can reduce or inhibit the enzymatic activity of the mosquitoes against classes of insecticides is a top priority to curb the resistance problem.
LLINs that use two unrelated insecticides or an insecticide plus a synergist have been shown to have increased efficacy against pyrethroid-resistant malaria vectors . The incorporation of the synergist, piperonyl butoxide (PBO), in LLINs is able to significantly reduce or inhibit the enzymatic detoxification of insecticides, thus increasing the toxicity against mosquitoes . PBO is an inhibitor of mixed-function oxidases implicated in pyrethroid resistance and also increases the rate of insecticide uptake through the mosquito cuticle [11, 16]. There are currently two pyrethroid synergist LLINs recommended by the WHO, namely, Olyset® Plus and PermaNet® 3.0 . The latter is a combination of deltamethrin coated on the net’s polyester side panels and a mixture of deltamethrin and PBO on the polyethylene top panel.
In this study, we compared the pyrethroid synergist PermaNet® 3.0 LLIN, the pyrethroid-only PermaNet® 2.0 LLIN and an untreated net, following standard WHO procedures . This was done to determine the comparative efficacy against a free-flying, wild population of An. gambiae mosquitoes. As per recommended WHO standard experimental hut trials measurable outcomes, efficacy was measured in terms of blood-feeding inhibition, deterrence, induced exophily and mortality (both immediately and after 24 h).
The PermaNet test was conducted in Lower Moshi rice irrigation schemes in northern Tanzania using an East African experimental hut design. The experimental huts used in this trial were situated in Mabogini village, Moshi Rural District, northern Tanzania. They were constructed according to an East African experimental hut design first described elsewhere [17, 21]. The study area was chosen because of its high mosquito density throughout the year and a well-known status of insecticide resistance of the malaria vectors, An. arabiensis. Malaria vectors in this area are currently resistant to pyrethroids [14, 22, 23].
Before washing each LLIN, 20 g of Persil Savon de Marseille (Unilever) was added to 10 l of dechlorinated water and dissolved for 30 min. Each net was washed, immersed in the soap solution and manually agitated by hand protected with gloves for 10 min for an average of 20 rotations per minute. Nets were thereafter rinsed twice in dechlorinated tap water and dried in the shade. After been dried, the nets were stored in a dark room at ambient temperature. PermaNet® 2.0 and PermaNet® 3.0 LLINs were washed 20 times, while untreated nets were washed the same.
A susceptibility test was conducted using the commonly-used pyrethroids, deltamethrin (0.05%) and permethrin (0.75%). Susceptibility tests were done following the procedures defined in the WHO Pesticide Evaluation Scheme (WHOPES) protocol.  Mosquitoes population was considered susceptible when mortality was between 98 and 100%. A mortality rate of less than 98% suggested the existence of a resistant population . If the mortality rate was less than 90%, it indicated the existence of a resistance gene in the population against the evaluated insecticide [6, 20].
Rectangular PermaNet® 2.0 and PermaNet® 3.0 LLINs were provided by their manufacturer, Vestergaard Frandsen SA, Denmark. Untreated nets were purchased from local shops; they were rectangular polyester nets (manufactured by A to Z Textile Mills, Arusha, Tanzania (http://www.azpfl.com/index.php/en/)), white in colour with no insecticide treatment. The PermaNet® 2.0 was polyester and coated with 55 mg/m2 ± 25% deltamethrin. The PermaNet® 3.0 had a polyethylene roof with 2.8 g/kg ± 25% deltamethrin and 4.0 g/kg ± 25% PBO, and sides coated with 2.8 g/kg ± 25% deltamethrin. PBO is a synergist compound that elevates the rate of penetration of the insecticide into the insect cuticle  and inhibits the enzymatic ability of the insect to breakdown the insecticide .
Bioassays were conducted for all nets before and after washing. Bioassays were also conducted for nets that were washed 20 times before the experimental hut trial commenced and for all nets (washed and unwashed) after the experimental hut trial ended. The cone bioassays were executed for the roof, two long sides and two shots sides (legs and head positions of the nets). Five replicates were taken for each bioassay. All net samples were folded in aluminium foil and placed individually in a labelled clean black plastic bag prior to the assays being conducted.
Bioassays on mosquito nets
The standard WHO method for cone bioassays was followed to determine the bioefficacy of LLINs against field-derived populations, permethrin-selected population and susceptible laboratory-reared Anopheles gambiae s.s. (Kisumu strain) . The Kisumu colony was established at the Tropical Pesticides Research Institute (TPRI) in 1992. The colony is 100% susceptible to all approved WHOPES pesticides, which are tested frequently and confirmed every 6 months for susceptibility status using the standard WHO susceptibility test.
At the TPRI insectary, five unfed An. gambiae s.s. females were exposed for three minutes, removed and kept in holding paper cups provided with 10% sugar solution. The knockdown rate was recorded at 60 min post-exposure and the mortality rate after 24 h. Two cone tests were performed for each side of the net and for each mosquito population including for the laboratory-susceptible population; 250 mosquitoes of each of the five populations were tested for each net type. Mosquitoes exposed to untreated nets were used as controls and all results in control with mortality rates above 20% were discarded. Corrected mortality was applied when control mortality was above 5% using the Abbott’s formula.
Experimental hut trial study design
The following five treatment arms were compared: (i) unwashed PermaNet® 2.0 (P2.0UN); (ii) PermaNet® 2.0 washed 20 times (P2.0WA); (iii) unwashed PermaNet® 3.0 (P3.0UN); (iv) PermaNet® 3.0 washed 20 times (P3.0WA); and (v) untreated polyester net (UTN). Each net was punctured with six (4 cm × 4 cm) holes to simulate a community-used worn net. The treatment arms were rotated five times through the huts using 5 by 5 Latin square design.
A treatment was assigned to a particular hut for five nights before being rotated to the next hut. In each hut, there was a male volunteer who gave consent to participate in the study before the trial began. Based on the treatment arms, five sleepers were randomly rotated during the five nights in five huts. Five sleepers were rotated through five huts on consecutive nights. Five nets were available per treatment arm and each net was tested on a consecutive week during the 5 weeknight rotations. At the end of each rotation, the huts were cleaned and aired for 1 day and the treatments moved to the next hut. White sheets were laid over the veranda and floors in the rooms to ease the collection of knocked-down mosquitoes. Each morning after dawn, mosquitoes were collected using aspirators from the floor, walls, veranda traps and inside the nets, scored as dead or alive and as fed or unfed, and identified to species using an Olympus BX41microscope (Olympus Corporation, Rochester, NY, USA). Live mosquitoes were kept for 24 h in paper cups with sugar solution to determine delayed mortality.
The main outcomes measured were: deterrence (defined as a reduction in hut entry relative to the control huts fitted with untreated nets); treatment-induced exophily (defined as the proportion of mosquitoes found in exit traps relative to the control huts); blood-feeding inhibition (defined as the proportional reduction in blood-feeding mosquitoes relative to untreated nets); and mortality (defined as the proportion of mosquitoes found dead).
The deterrence and blood-feeding inhibition of these outcomes are indicators of the personal protection rate, which can be estimated by the equation:
where Bu = is the total number of blood-fed mosquitoes in the huts with untreated nets and Bt is the total number of blood-fed mosquitoes in the huts with treated nets.
The overall killing effect of the treatment was estimated by the equation:
where Kt is the number of mosquitoes killed in the huts with treated nets, Ku is the number of mosquitoes found dying in the huts with untreated nets and Tu is the total number of mosquitoes collected from the huts with untreated nets.
The criteria for approval of PermaNet® 3.0 was that, the PermaNet® 3.0 LLINs that were washed 20 times or more should perform equal to or better than a conventionally treated washed net just before exhaustion. Twenty washes are set by the WHO as the average number of washes a LLIN is likely to incur during its life, assuming nets are washed 4 times a year and last 3 to 5 years.
For cone bioassays, knockdown and mortalities were compared for individual samples using regression analyses. Data, aggregated for mosquito population, net type and net section, were assessed using logistic regression for proportional data outcomes (proportions of blood-feeding and dying mosquitoes and those exiting the hut each night). All data for each net were then combined for net sections.
Cone bioassay with susceptible mosquitoes
The knockdown effect for the treated nets 60 min after exposure was 100%, while the mortality rate after 24 h was 100%. The untreated net knockdown effect and mortality rate was 0% (see Fig. 1a and b).
After 20 washes
After 20 washes, the knockdown effect varied between the nets: in untreated nets, it was 0.0%, in P3.0WA it was 98.0% and in P2.0WA it was 92.8%. The mortality rate after 24 h was 0%, 100% and 100% for the untreated net, P3.0WA and P2.0WA, respectively (see Fig. 1a and b).
After the experimental hut trial
The washed, unwashed and untreated nets showed variations in both the knockdown and mortality rates after the experimental hut trial. The knockdown effect 60 min after exposure was 0%, 100%, 98%, 98% and 96%, while the mortality rate after 24 h was 0%, 96%, 98%, 98% and 94% for UTN, P3.0UN, P2.0UN, P2.0WA and P3.0WA, respectively (see Fig. 1a and b).
Cone bioassays with a resistant colony
After 20 washes
The knockdown effect of nets washed 20 times varied. The knockdown effect was 0%, 100% and 100% after 60 min for UTN, P3.0WA and P2.0WA, respectively. The mortality rate after 24 h was 0%, 100% and 94.4% for UTN, P3.0WA and P2.0WA, respectively (see Fig. 2a and b).
After the experimental hut trial
The nets’ efficacy after the hut trial varied considerably. The knockdown effect 60 min after exposure was 0.0%, 100.0%, 100.0%, 99.2% and 94.4%, while the mortality rate after 24 h was 0.0%, 100.0%, 100.0%, 98.4% and 92.8% for UTN, P3.0UN, P3.0WA, P2.0UN and P2.0WA, respectively (see Fig. 2a and b).
Deltamethrin-susceptibility test using wild and laboratory-reared mosquito populations
For the wild-caught adult female An. gambiae mosquitoes exposed to deltamethrin-treated WHO kit, the mortality rate was found to be 28.8%. Meanwhile, the survival rate was found to be 71.2% 24 h after exposure to WHOPES insecticide-treated paper. The mortality rate for the laboratory colony of An. gambiae s.s. was 100% against deltamethrin.
Permethrin-susceptibility test using wild and laboratory-reared mosquito populations
For the adult female An. gambiae mosquitoes exposed to permethrin-treated WHO kit, the mortality rate was found to be 29.0%. Meanwhile, the survival rate was found to be 71.0% 24 h after exposure to WHOPES insecticide-treated paper. The mortality for An. gambiae s.s laboratory colony (control) was 100% against deltamethrin.
Experimental hut trial
In the experimental hut trial, the efficacy of the evaluated nets was measured using the following parameters (see Table 1):
Deterrence: The rate of deterrence of mosquitoes was 78.7%, 78.7%, 80.0% and 86.7% for P2.0WA, P3.0UN, P3.0WA and P2.0UN, respectively.
Exophily: The number of mosquitoes found exiting the huts as the repellence effect of the LLINs treated nets varied from each due to different washing and brands. Exophily was found to be 9.3%, 90.0%, 93.8%, 81.3% and 80.0% for UTN, P2.0UN, P2.0WA, P3.0UN and P3.0WA, respectively.
Blood-feeding inhibition: Blood-feeding inhibition was found to be 100% for all treated nets as compared to the control.
Mortality: The corrected mortality due to mortality exceeded 5% in control for mosquitoes collected in the huts after 24 h was 59.5% for P2.0UN, 36.7% for P2.0WA, 49.3% for P3.0UN and 32.4% for P3.0WA.
Personal protection rate and killing effect rate of nets
An. gambiae species composition
All identified specimens of An. gambiae s.l. were found to belong to the An. arabiensis species (see Fig. 4).
This study was conducted in Lower Moshi, in which a wild population of An. gambiae mosquitoes has been identified as having both phenotypic and metabolic resistance to insecticides [14, 22, 23, 25]. The study site has an An. arabiensis population. This scenario was previously reported by Ijumba and others in the early 1990s, when they found a composition of 95% An. arabiensis . Another study conducted between 2010 and 2012 by Matowo and others found out of the 100% of mosquitoes in this area, 98% are of the An. arabiensis .
This study demonstrated that both unwashed LLINs and LLINs washed 20 times provided a high personal protection against An. arabiensis mosquitoes, which were found to be pyrethroid-tolerant according to the criteria provided by the WHO protocol for susceptibility test.  The nets were punctured to mimic community-used nets, but they still showed a great protection efficacy in spite of the holes. The personal protection rate for both unwashed LLINs and LLINs washed 20 times was found to be 100%. This is higher than what was reported in a previous study by Kitau and others, who tested intact nets . This suggests that in an area where there is a population of resistant vectors, a person can be protected against mosquitoes if positioned under a bed net, but is vulnerable when outside the bed net . Alternative personal protection tools other than bed nets, such as repellents, should be used for improved protection .
The differences in mortality rates might be attributed to phenotypic, knockdown resistance (kdr) or biochemical resistance mechanisms, as the mortality rates observed were very low [14, 22, 23, 29]. Similar scenario of low mortality was observed in areas with P450 and kdr resistance mechanisms, which have hampered the resistance rate among malaria vector control including An. funestus in South Africa where deltamethrin has been used intensively for IRS [30, 31]. In Cameroon, it was found that an evaluation of P450 activity in An. gambiae mosquitoes reduces the bioefficacy of permethrin-treated nets conducted in the laboratory [32, 33]. A combination of resistance mechanisms might be a major blocking factor to the control of malaria vectors by impairing the efficacy of combined insecticides or synergist such as PBO with insecticide . In the study area, the predominant mechanisms are phenotypic and metabolic [22, 23, 35].
Both PermaNet® 2.0 (P2.0WA) and PermaNet® 3.0 (P3.0UN) were found to have lowest deterrence effects (78.0%) while P2.0UN had highest deterrence (86.7%). The washing effect could not be seen in terms of decrease of deterrence effect in PermaNet 3.0 but in PermaNet 2.0. However, the reduction in the mosquito numbers entering the hut or house increases the possibility of personal protection, but may not be a reliable indicator of LLIN efficacy as sometimes variation in protection efficacy have been observed with similar nets . In Benin, the protection efficiency of an insecticide-treated net was found to be reduced to 50% in an area with a resistant population of An. gambiae mosquitoes, while in susceptible areas it was 100% . These findings indicate that PermaNet® 2.0 and improved PermaNet® 3.0 (with PBO) are advanced tools for protection against resistant populations of An. gambiae mosquitoes [8, 17, 37]. This efficacy has also been observed in Ethiopia  and Cote d’Ivoire . A similar study conducted in Muheza, Tanzania found that the personal protection rates for PermaNet® 3.0 and PermaNet® 2.0 washed 20 times were 71 and 73%, respectively . The cause of these variations in the personal protection rate between and within the two PermaNet brands done in Tanzania are still not well understood. But it has been suggested that they are attributed to the differences in insecticide resistance among wild mosquito populations and may be their different resistance mechanisms involved [17, 23, 29].
The mortality rates after use of either the washed or unwashed PermaNet® 2.0 and PermaNet® 3.0 LLINs were found to be between 32.4 and 59.5%. Low mortality rates have been recorded with deltamethrin-treated nets elsewhere including in Cote d’Ivoire, Southern Benin and Burkina Faso, which are all areas with mosquito populations that have a reduced susceptibility to permethrin and deltamethrin; mortality was below 40% in all those three areas mentioned above [31, 36]. The incorporation of deltamethrin and PBO in nets has been found to improve the mortality rates of mosquitoes in areas with highly-resistant populations due to the synergistic effect [38–40]. PBO has been found to increase the cuticle penetration rate of insecticides, hence increasing the mortality rate of the targeted species by increasing insecticide toxicity [22, 41]. It has been reported that deterrence varies widely from 0 to 70% during huts rotation for similar LLINs against wild resistant An. gambiae populations .
Natural exophily was found to be 9.3% for untreated nets, while it was >80.0% for the treated washed and unwashed PermaNet® 2.0 and PermaNet® 3.0 LLINs. Despite of resistance level of wild population of An. arabiensis against deltamethrin still induced exophily by both brands of PermaNet either washed or unwashed was higher and blood-feeding inhabitation was 100%. The deltamethrin resistance level has increased significantly in the past 10 years in Lower Moshi [14, 22, 23, 35].
Although the nets were holed to mimic community-used nets, the PermaNet® 3.0 and 2.0 still had irritancy effect to hold off An. arabiensis not feeding on volunteer under the bed net In Cote d’Ivoire, a resistant wild population of An. gambiae mosquitoes was found to have low feeding succession rates, but it might have been due to intact (not holed) nets being utilised .
The present study reveals that the use of both unwashed and washed PermaNet® 2.0 LLINs was associated with higher mortality rates than with the PermaNet® 3.0 LLINs. Exophily and deterrence rates were similar. A community-based evaluation of PermaNet® 3.0 and PermaNet® 2.0 LLINs in an area with a similar level or a higher phenotypic and metabolic resistance in mosquitoes will allow for comparable results and thus for a better conclusion.
The observed impact of the unwashed PermaNet® 3.0 LLIN compared to the unwashed PermaNet® 2.0 LLIN was confirmed to be higher in terms of the killing effect (70% versus 50%, respectively). Similar results were obtained for the washed PermaNet 2.0® and PermaNet® 3.0. This low killing effect was associated with an elevated resistance to pyrethroid among the wild mosquito population [25, 42]. The highest deterrence effect, personal protection and feeding inhibition was the most outstanding factor to advocates these nets use in areas with elevated insecticides resistance.
Indoor residual spray
Long-lasting insecticidal net
PermaNet® 2.0 unwashed net
PermaNet® 2.0 net washed 20 times
PermaNet® 3.0 unwashed net
PermaNet® 3.0 net washed 20 times
Tropical Pesticides Research Institute
World Health Organization
WHO Pesticide Evaluation Scheme
Wanjala CL, Zhou G, Mbugi J, Simbauni J, Afrane YA, Ototo E, Gesuge M, Atieli H, Githeko AK, Yan G. Insecticidal decay effects of long-lasting insecticide nets and indoor residual spraying on Anopheles gambiae and Anopheles arabiensis in Western Kenya. Parasit Vectors. 2015;8:588.
Asale A, Getachew Y, Hailesilassie W, Speybroeck N, Duchateau L, Yewhalaw D. Evaluation of the efficacy of DDT indoor residual spraying and long-lasting insecticidal nets against insecticide resistant populations of Anopheles arabiensis Patton (Diptera: Culicidae) from Ethiopia using experimental huts. Parasit Vectors. 2014;7:131.
Aïkpon R, Sèzonlin M, Tokponon F, Okè M, Oussou O, Oké-Agbo F, Beach R, Akogbéto M. Good performances but short lasting efficacy of Actellic 50 EC Indoor Residual Spraying (IRS) on malaria transmission in Benin, West Africa. Parasit Vectors. 2014;7:256.
Deressa W, Yihdego YY, Kebede Z, Batisso E, Tekalegne A, Dagne GA. Effect of combining mosquito repellent and insecticide treated net on malaria prevalence in Southern Ethiopia: a cluster-randomised trial. Parasit Vectors. 2014;7:132.
WHO. World malaria report 2014. Geneva: WHO; 2015.
WHO. Guidelines for laboratory and field testing of long-lasting insecticidal mosquito nets. WHO/CDS/WHOPES/GCDPP/2005.11. 2005.
WHO. Test Procedures for Insecticide Resistance Monitoring in Malaria Vector Mosquitoes. Geneva: World Health Organization; 2013. http://www.who.int/malaria/publications/atoz/9789241505154/en/.
Okia M, Ndyomugyenyi R, Kirunda J, Byaruhanga A, Adibaku S, Lwamafa DK, Kironde F. Bioefficacy of long-lasting insecticidal nets against pyrethroid-resistant populations of Anopheles gambiae s.s. from different malaria transmission zones in Uganda. Parasit Vectors. 2013;6:130.
Yewhalaw D, Asale A, Tushune K, Getachew Y, Duchateau L, Speybroeck N. Bio-efficacy of selected long-lasting insecticidal nets against pyrethroid resistant Anopheles arabiensis from South-Western Ethiopia. Parasit Vectors. 2012;5:159.
Haji K, Khatib B, Smith S, Ali A, Devine G, Coetzee M, Majambere S. Challenges for malaria elimination in Zanzibar: pyrethroid resistance in malaria vectors and poor performance of long-lasting insecticide nets. Parasit Vectors. 2013;6:82.
Ahmad M, Denholm I, Bromilow RH. Delayed cuticular penetration and enhanced metabolism of deltamethrin in pyrethroid-resistant strains of Helicoverpa armigera from China and Pakistan. Pest Manag Sci. 2006;62:805–10.
Ranson H, Jensen B, Wang X, Prapanthadara L, Hemingway J, Collins FH. Genetic mapping of two loci affecting DDT resistance in the malaria vector Anopheles gambiae. Insect Mol Biol. 2000;9:499–507.
Van Bortel W, Chinh VD, Berkvens D, Speybroeck N, Trung HD, Coosemans M. Impact of insecticide-treated nets on wild pyrethroid resistant Anopheles epiroticus population from southern Vietnam tested in experimental huts. Malar J. 2009;8:248.
Kabula B, Tungu P, Matowo J, Kitau J, Mweya C, Emidi B, Masue D, Sindato C, Malima R, Minja J, et al. Susceptibility status of malaria vectors to insecticides commonly used for malaria control in Tanzania. Trop Med Int Health. 2012;17:742–50.
Djenontin A, Chabi J, Baldet T, Irish S, Pennetier C, Hougard J-M, Corbel V, Akogbeto M, Chandre F. Managing insecticide resistance in malaria vectors by combining carbamate-treated plastic wall sheeting and pyrethroid-treated bed nets. Malar J. 2009;8:233.
WHO. Global Plan for insecticide resistance management in malaria vector. Geneva: Roll back malaria; 2012.
Tungu P, Magesa S, Maxwell C, Malima R, Masue D, Sudi W, Myamba J, Pigeon O, Rowland M. Evaluation of PermaNet 3.0 a deltamethrin-PBO combination net against Anopheles gambiae and pyrethroid resistant Culex quinquefasciatus mosquitoes: an experimental hut trial in Tanzania. Malar J. 2010;9:21.
Koudou B, Koffi A, Malone D, Hemingway J. Efficacy of PermaNet(R) 2.0 and PermaNet(R) 3.0 against insecticide-resistant Anopheles gambiae in experimental huts in Cote d’Ivoire. Malar J. 2011;10:172.
WHO recommended long-lasting insecticidal nets. http://www.who.int/whopes/Long_lasting_insecticidal_nets_06_Feb_2014.pdf?ua=1. Accessed 30 May 2016.
WHO. Guidelines for laboratory and field-testing of long-lasting insecticidal nets. WHO/HTM/NTD/WHOPES/2013.3. Geneva; World Health Organisation. 2013.
Smith A. A verandah-trap hut for studying the house-frequenting habits of mosquitos and for assessing insecticides. 2. The effect of dichlorvos (DDVP) on egress and mortality of Anopheles gambiae Giles and Mansonia uniformis (Theo.) entering naturally. Bull Entomol Res. 1965;56:275–82.
Matowo J, Kulkarni M, Mosha F, Oxborough R, Kitau J, Tenu F, Rowland M. Biochemical basis of permethrin resistance in Anopheles arabiensis from Lower Moshi, north-eastern Tanzania. Malar J. 2010;9:193.
Kabula B, Tungu P, Malima R, Rowland M, Minja J, Wililo R, Ramsan M, McElroy PD, Kafuko J, Kulkarni M, Protopopoff N, Magesa S, Mosha F, Kisinza W. Distribution and spread of pyrethroid and DDT resistance among the Anopheles gambiae complex in Tanzania. Med Vet Entomol. 2014;28:244–52.
Bingham G, Gunning RV, Gorman K, Field LM, Moores GD. Temporal synergism by microencapsulation of piperonyl butoxide and α-cypermethrin overcomes insecticide resistance in crop pests. Pest Manag Sci. 2007;63(3):276–81.
Mahande AM, Dusfour I, Matias JR, Kweka EJ. Knockdown Resistance, rdl Alleles, and the Annual Entomological Inoculation Rate of Wild Mosquito Populations from Lower Moshi, Northern Tanzania. J Global Infect Dis. 2012;4:114–9.
Ijumba J, Shenton F, Clarke S, Mosha F, Lindsay S. Irrigated crop production is associated with less malaria than traditional agricultural practices in Tanzania. Trans Royal Soc Trop Med Hyg. 2002;96:476–80.
Kitau J, Oxborough R, Kaye A, Chen-Hussey V, Isaacs E, Matowo J, Kaur H, Magesa SM, Mosha F, Rowland M, et al. Laboratory and experimental hut evaluation of a long-lasting insecticide treated blanket for protection against mosquitoes. Parasit Vectors. 2014;7:1–12.
Darriet F, Chandre F. Combining Piperonyl Butoxide and Dinotefuran Restores the Efficacy of Deltamethrin Mosquito Nets Against Resistant Anopheles gambiae (Diptera: Culicidae). J Med Entomol. 2011;48:952–5.
Kabula B, Tungu P, Malima R, Rowland M, Minja J, Wililo R, Ramsan M, McElroy PD, Kafuko J, Kulkarni M, et al. Distribution and spread of pyrethroid and DDT resistance among the Anopheles gambiae complex in Tanzania. Med Vet Entomol. 2014;28:244–52.
Tokponnon F, Aholoukpe B, Denon E, Gnanguenon V, Bokossa A, N’guessan R, Oke M, Gazard D, Akogbeto M. Evaluation of the coverage and effective use rate of long-lasting insecticidal nets after nation-wide scale up of their distribution in Benin. Parasit Vectors. 2013;6:265.
N’Guessan R, Boko P, Odjo A, Chabi J, Akogbeto M, Rowland M. Control of pyrethroid and DDT-resistant Anopheles gambiae by application of indoor residual spraying or mosquito nets treated with a long-lasting organophosphate insecticide, chlorpyrifos-methyl. Malar J. 2010;9:44.
Chouaibou M, Simard F, Chandre F, Etang J, Darriet F, Hougard JM. Efficacy of bifenthrin-impregnated bednets against Anopheles funestus and pyrethroid-resistant Anopheles gambiae in North Cameroon. Malar J. 2006;5:77.
Etang J, Chandre F, Guillet P, Manga L. Reduced bio-efficacy of permethrin EC impregnated bednets against an Anopheles gambiae strain with oxidase-based pyrethroid tolerance. Malar J. 2004;3:46.
Ochomo E, Bayoh NM, Kamau L, Atieli F, Vulule J, Ouma C, Ombok M, Njagi K, Soti D, Mathenge E, et al. Pyrethroid susceptibility of malaria vectors in four Districts of western Kenya. Parasit Vectors. 2014;7:310.
Kulkarni M, Rowland M, Alifrangis M, Mosha F, Matowo J, Malima R, Peter J, Kweka E, Lyimo I, Magesa S, et al. Occurrence of the leucine-to-phenylalanine knockdown resistance (kdr) mutation in Anopheles arabiensis populations in Tanzania, detected by a simplified high-throughput SSOP-ELISA method. Malar J. 2006;5:56.
N’Guessan R, Corbel V, Akogbeto M, Rowland M. Reduced efficacy of insecticide-treated nets and indoor residual spraying for malaria control in pyrethroid resistance area, Benin. Emerg Infect Dis. 2007;13:199–206.
Okumu F, Mbeyela E, Lingamba G, Moore J, Ntamatungiro A, Kavishe D, Kenward M, Turner E, Lorenz L, Moore S. Comparative field evaluation of combinations of long-lasting insecticide treated nets and indoor residual spraying, relative to either method alone, for malaria prevention in an area where the main vector is Anopheles arabiensis. Parasit Vectors. 2013;6:46.
Corbel V, Chabi J, Dabiré RK, Etang J, Nwane P, Pigeon O, Akogbeto M, Hougard J-M. Field efficacy of a new mosaic long-lasting mosquito net (PermaNet® 3.0) against pyrethroid-resistant malaria vectors: a multi centre study in Western and Central Africa. Malar J. 2010;9:133.
Pennetier C, Bouraima A, Chandre F, Piameu M, Etang J, Rossignol M, Sidick I, Zogo B, Lacroix M-N, Yadav R, et al. Efficacy of Olyset® Plus, a New Long-Lasting Insecticidal Net Incorporating Permethrin and Piperonil-Butoxide against Multi-Resistant Malaria Vectors. PLoS ONE. 2013;8:e75134.
N’Guessan R, Asidi A, Boko P, Odjo A, Akogbeto M, Pigeon O, Rowland M. An experimental hut evaluation of PermaNet® 3.0, a deltamethrin–piperonyl butoxide combination net, against pyrethroid-resistant Anopheles gambiae and Culex quinquefasciatus mosquitoes in southern Benin. Trans R Soc Trop Med Hyg. 2010;104:758–65.
Kasai S, Komagata O, Itokawa K, Shono T, Ng LC, Kobayashi M, Tomita T. Mechanisms of Pyrethroid Resistance in the Dengue Mosquito Vector, Aedes aegypti: Target Site Insensitivity, Penetration, and Metabolism. PLoS Negl Trop Dis. 2014;8:e2948.
Matowo J, Jones CM, Kabula B, Ranson H, Steen K, Mosha F, Rowland M, Weetman D. Genetic basis of pyrethroid resistance in a population of Anopheles arabiensis, the primary malaria vector in Lower Moshi, north-eastern Tanzania. Parasit Vectors. 2014;7:274.
The authors wish to acknowledge Richard Oxborough and Jovin Kitau of the Vector Control Group at the Kilimanjaro Christian Medical Center for supervising the trial. The authors also acknowledge the hut sleepers who volunteered after signing the written consent form.
The study was financially supported by Vestergaard Frandsen, Aarhus, Denmark. The funding body had no influence on this publication.
Availability of data and materials
The dataset supporting the conclusions of this paper is included within the paper.
EJK conceived, designed and analysed the data. LJL and AMM collected the data. EJK, LJL and AMM drafted the paper and revised it extensively. All authors agreed upon the submission of the paper.
The authors declare that they have no competing interests.
Consent for publication
Ethics approval and consent to participate
This study was approved by the TPRI, which regulates pesticide-related studies in Tanzania. All hut sleepers gave written consent for participating in the study, which was witnessed by a person who was not involved in the study.
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Kweka, E.J., Lyaruu, L.J. & Mahande, A.M. Efficacy of PermaNet® 3.0 and PermaNet® 2.0 nets against laboratory-reared and wild Anopheles gambiae sensu lato populations in northern Tanzania. Infect Dis Poverty 6, 11 (2017) doi:10.1186/s40249-016-0220-z
- Long-lasting insecticidal nets
- Anopheles gambiae
- Experimental hut
- Personal protection rate