1999
DOI: 10.1054/tuld.1999.0204
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Association of functional mutant homozygotes of the mannose binding protein gene with susceptibility to pulmonary tuberculosis in India

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Cited by 93 publications
(68 citation statements)
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“…The B allele frequency in the controls of the present study (0·11) is similar to that reported earlier for Indian control individuals (0·11) and comparable to that reported for Caucasians, Chinese and Eskimos (0·11-0·17) [33,34]. The frequency of the D allele in our study (0·01) is also comparable with the earlier frequency reported in Indian individuals (0·04) and to that of Caucasians (0·05) and Africans (0·05) [33][34][35][36]. Also, the frequency of the C allele in the present study (0·08) is comparable to that reported earlier in Indian individuals (0·03) and also to Caucasians (0·02), but lower than in Africans (0·23-0·29) [35].…”
Section: Discussionsupporting
confidence: 81%
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“…The B allele frequency in the controls of the present study (0·11) is similar to that reported earlier for Indian control individuals (0·11) and comparable to that reported for Caucasians, Chinese and Eskimos (0·11-0·17) [33,34]. The frequency of the D allele in our study (0·01) is also comparable with the earlier frequency reported in Indian individuals (0·04) and to that of Caucasians (0·05) and Africans (0·05) [33][34][35][36]. Also, the frequency of the C allele in the present study (0·08) is comparable to that reported earlier in Indian individuals (0·03) and also to Caucasians (0·02), but lower than in Africans (0·23-0·29) [35].…”
Section: Discussionsupporting
confidence: 81%
“…A recent study on animal models of Afuinduced asthma by Hogaboam et al [32] showed that in Afusensitized murine MBL-A-deficient mice whole lung T helper cell type 2 cytokine levels were decreased significantly, and whole lung interferon-gamma levels were increased significantly when compared with normal mice, indicating that the murine MBL-A contributes to the development and maintenance of airway hyperresponsiveness. As well as the novel intronic SNP, the three exon 1 SNPs [G875A (B allele), G884A (C allele) and C868T (D allele)] at codons 54, 57 and 52, respectively, leading to low plasma MBL levels that have been reported in other populations including the Indian population, were also present in our study population [13,[33][34][35][36]. The B allele frequency in the controls of the present study (0·11) is similar to that reported earlier for Indian control individuals (0·11) and comparable to that reported for Caucasians, Chinese and Eskimos (0·11-0·17) [33,34].…”
Section: Discussionmentioning
confidence: 59%
“…The high incidence of heterozygosity for the structural variants in many populations throughout the world 9,10 suggests that there may be a selective advantage for heterozygotes; moreover, individuals heterozygous for B, C and D may be protected against certain pathogens, especially intracellular microorganisms (ie, Mycobacteria spp and Leishmania spp. [21][22][23][24][25][26][27] The fact that there are only seven common haplotypes (eg, HYPA, HYPD, LXPA, LYPA, LYPB, LYQA and LYQC) further supports the role for recent selective pressure on MBL2. MBL deficiency, measured as low serum levels, has been associated with susceptibility to infection in children and adults.…”
mentioning
confidence: 99%
“…167 However, no associations have been reported between leprosy susceptibility and MBL2 variants, and in contradiction to the above reports, MBL2 variants were found with increased frequency in a limited Indian pulmonary tuberculosis study. 168 …”
mentioning
confidence: 99%