| Literature DB >> 29273010 |
Udeshika Lakmini Kariyawasam1, Angamuthu Selvapandiyan2, Keshav Rai3, Tasaduq Hussain Wani2, Kavita Ahuja2, Mizra Adil Beg2, Hasitha Upendra Premathilake4, Narayan Raj Bhattarai3, Yamuna Deepani Siriwardena1, Daibin Zhong5, Guofa Zhou5, Suman Rijal3, Hira Nakhasi6, Nadira D Karunaweera7.
Abstract
BACKGROUND: Leishmania donovani is the etiological agent of visceral leishmaniasis (VL) in the Indian subcontinent. However, it is also known to cause cutaneous leishmaniasis (CL) in Sri Lanka. Sri Lankan L. donovani differs from other L. donovani strains, both at the molecular and biochemical level. To investigate the different species or strain-specific differences of L. donovani in Sri Lanka we evaluated sequence variation of the kinetoplastid DNA (kDNA).Entities:
Keywords: Antimony resistance; Geographical clustering; Haplotype diversity; India; Nepal; Phenotypic characteristics; Skin lesions; Visceral leishmaniasis; kDNA minicircle sequences
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Year: 2017 PMID: 29273010 PMCID: PMC5741890 DOI: 10.1186/s12879-017-2883-x
Source DB: PubMed Journal: BMC Infect Dis ISSN: 1471-2334 Impact factor: 3.090
Fig. 1Geographical distribution of leishmaniasis patients in Sri Lanka included in the study. The geographical origin of leishmaniasis patients within the main administrative provinces of the country are shown () with the number of patients from each province given within parenthesis. SL-CL-S: patients with uncomplicated cutaneous leishmaniasis, SL-CL-DR: patients with cutaneous leishmaniasis that showed poor response to antimony therapy and SL-VL: visceral leishmaniasis patients
Genetic diversity parameters of Leishmania donovani isolates from Sri Lanka, India and Nepal
| Origin | Sri Lanka | India | Nepal |
|---|---|---|---|
| Haplotype diversity ( | 0.757 | 0.889 | 0.725 |
| Nucleotide diversity ( | 0.034 | 0.093 | 0.128 |
| Number of sequences used (n) | 166 | 51 | 52 |
| Number of polymorphic sites(S) | 33 | 36 | 34 |
| Number of Haplotypes (h) | 43 | 8 | 5 |
| Tajima’s | −1.098(>0.1) | 1.197(>0.1) | 2.646(<0.01) |
| Fu’s | −25.801 (>0.02) | 10.780(<0.02) | 21.900(<0.02) |
Fu’s Fs: Not significant, P > 0.02. Tajima’s D: Not significant, P > 0.10
kDNA based genetic distances (F ) between populations of Leishmania parasites from selected geographical areas
| Sri Lanka | India | Nepal | |
|---|---|---|---|
| Sri Lanka | 0.000 | ||
| India | 0.347 | 0.000 | |
| Nepal | 0.522a | 0.236 | 0.000 |
aSignificant at level of 0.05
Diagonal: genetic distance within major geographic areas; below diagonal: genetic distance between populations
Fig. 2Phylogenetic tree constructed with the sequences of L. donovani isolates from Sri Lanka and other geographic locations. Ld-India-VL:L. donovani [India] (Bone marrow);Ld(DD8):L. donovani [India] (Bone marrow); SL-VL: Leishmania VL Sri Lankan isolates (Bone marrow); SL-CL-S:Leishmania CL Sri Lankan isolates (Skin); SL-CL-DR: Leishmania CL Sri Lankan isolates not respond to drug(Skin);Ld-Nepal: L.donovani[Nepal](Bone marrow); Li-Turkey: L. infantum[Turkey] (Spleen); Li-Spain:L. infantum [Spain] (Unknown);Ld-Peakin-China: L. donovani[China];Ld-France: L. donovani [France]
Fig. 3Phylogenetic trees with the Leishmania strains from Sri Lanka (SL), India (IN) and Nepal (NP) with (a) and /without (b) the global Leishmania reference panel consisting of different species of Leishmania from different regions. Lb(P):L. braziliensis [Peru] (Skin);Ld(DD8)/Ld(IN):L. donovani [India] (Bone marrow); Li(SP):L. infantum [Spain] (Unknown); Lm(A1):L. major [Libya]; Lt(TK):L. tropica [Turkey] (Skin); Lam: L. amazonenis (Skin); Li(TK):L. infantum [Turkey] (Spleen); SL-VL (52–55): VL Sri Lankan isolate (Bone marrow); SL_CL-S (2,3,6–8,10–14,16,17,31–46,48–50):Leishmania CL Sri Lankan isolate (Skin); SL_CL-DR (1,9,11,15,51,56):Leishmania CL Sri Lankan that failed to respond to antimonial drugs (Skin); IN-VL: L. donovani [India] (Bone marrow); IN-PKDL: Leishmania from post-kala azar dermal leishmaniasis (PKDL) [India] (Skin); NP-VL: Leishmania VL Nepalian isolate (Bone marrow); NP-PKDL:Leishmania cause PKDL [Nepal] (Skin)
Fig. 4Phylogenetic trees constructed with the sequences of Indian parasite isolates. a Phylogenetic tree constructed with the sequences of parasite isolates with the global reference panel. b Phylogenetic tree constructed for internal comparison of the sequences of parasite isolates. Lb(P):L. braziliensis [Peru] (Skin); Ld(DD8)/Ld(IN): L. donovani [India] (Bone marrow); Li(SP):L. infantum [Spain] (Unknown); Lm(A1):L. major [Libya]; Lt(TK):L. tropica [Turkey] (Skin); Lam: L. amazonenis (Skin); Li(TK):L. infantum [Turkey] (Spleen), IN-VL; L. donovani [India] (Bone marrow), IN-PKDL; Leishmania from PKDL [India] (Skin)
Fig. 5Phylogenetic trees constructed with the sequences of Nepal parasite isolates. a Phylogenetic tree constructed with the sequences of parasite isolates with the global reference panel. b Phylogenetic tree constructed for internal comparison of the sequences of parasite isolates. Lb(P): L. braziliensis [Peru] (Skin);Ld(DD8)/Ld(IN):L. donovani [India] (Bone marrow); Li(SP):L. infantum [Spain] (Unknown); Lm(A1):L. major [Libya]; Lt(TK):L. tropica [Turkey] (Skin); Lam:L. amazonenis (Skin); Li(TK):L. infantum [Turkey] (Spleen); NP-VL: Leishmania VL Nepalian isolate (Bone marrow); NP-PKDL: Leishmania cause PKDL [Nepal] (Skin)