Evidence for an early appearance of modern post-switch isotypes in mammalian evolution; cloning of IgE, IgG and IgA from the marsupialMonodelphis domestica

Aveskogh, Maria; Hellman, Lars

doi:10.1002/(sici)1521-4141(199809)28:09<2738::aid-immu2738>3.0.co;2-i

Cited by 63 publications

(29 citation statements)

References 44 publications

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“…A similar situation has also been observed for the heavy chain locus in many placental mammals. Duplications have been only rarely observed for the e chain, while multiple and relatively recent independent duplications seem to have resulted in multiple c chain genes [34]. Is there an advantage of having several C regions in the k chain locus, or is it only a way to create several J segments and thereby higher variability?…”

Section: Discussionmentioning

confidence: 99%

High variability in complementarity‐determining regions compensates for a low number of V gene families in the λ light chain locus of the platypus

Johansson¹,

Salazar²,

Aveskogh³

et al. 2005

Eur J Immunol

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Based on the analysis of a panel of variable (V) region sequences from the Australian duck-billed platypus and the Australian short beaked echidna, the monotremes were found to express a highly diversified Vk repertoire. High variability was observed both in sequence and in length of all three CDR regions. However, all monotreme sequences were found to form a separate branch on a distance tree, and the monotremes appear to express only two Vk gene families. The appearance of all Vk gene segments in one branch on the distance tree gives further support for the notion that deletions of entire V region clans or families, followed by successive rounds of gene duplications may be a relatively common phenomenon during vertebrate evolution. Four different constant region sequences were also identified and a preferential use of certain J segments to each constant region was observed. A more detailed picture of the locus was obtained by analysis of genomic DNA by Southern blot and PCR. The organization of the lambda locus involves multiple V and several constant region genes with one or several joining segments positioned upstream of each constant region, similar to the organization in mouse and man. An mRNA frequency analysis shows that the k light chain accounts for more than 90% of the light chain transcripts in the spleen. The abundance and the high variability indicate that light chain diversity at the k locus contributes significantly to the antigen-binding repertoire in monotremes. A high k to j light chain ratio also indicates that variability in the CDR regions is more important for the repertoire size than the total number of V gene families.

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Section: Discussionmentioning

confidence: 99%

High variability in complementarity‐determining regions compensates for a low number of V gene families in the λ light chain locus of the platypus

Johansson¹,

Salazar²,

Aveskogh³

et al. 2005

Eur J Immunol

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“…The genes for the heavy chain of IgA have been cloned from several species, including humans (Flanagan et al, 1984), nonhuman primates (Kawamura et al, 1989(Kawamura et al, , 1990Ueda et al, 1988;Scinicariello et al, 2006;Rogers et al, 2008), rodents (Tucker et al, 1981;Bruggemann et al, 1986), bats (Butler et al, 2011), pets and domesticated animals (Knight et al, 1988;Burnett et al, 1989;White et al, 1998;Brown and Butler, 1994;Wagner et al, 1997;Patel et al, 1995;Zhou et al, 2006), dolphins (Mancia et al, 2007), marsupials (Aveskogh and Hellman, 1998), monotremes (Belov et al, 2002;Vernersson et al, 2010), and birds (Mansikka, 1992;Magor et al, 1998;Choi et al, 2010;Huang et al, 2012;Guo et al, 2014), in some cases as part of species genome projects. Thus, DNA sequence information for IgA is available for a wide range of mammalian and an increasing number of bird species.…”

Section: Iga Heavy Chain Genesmentioning

confidence: 99%

Mucosal Immunoglobulins

Woof

2015

Mucosal Immunology

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“…Partial cDNA clones of the ⑀-and ␥-chains were isolated by PCR using degenerated primers. The design and sequence of the primers have been described previously (21). Purified ⑀-and ␥-chain fragments were labeled with 32 P by random priming (Megaprime; Amersham) and used as probes in the platypus library.…”

Section: Construction Of a Platypus Spleen Cdna Librarymentioning

confidence: 99%

Heavy Chain V Region Diversity in the Duck-Billed Platypus (Ornithorhynchus anatinus): Long and Highly Variable Complementarity-Determining Region 3 Compensates for Limited Germline Diversity

Johansson

Aveskogh

Munday

et al. 2002

The Journal of Immunology

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In this work, to study the emergence of the H chain V region repertoire during mammalian evolution, we present an analysis of 25 independent H chain V regions from a monotreme, the Australian duck-billed platypus, Ornithorhynchus anatinus. All the sequences analyzed were found to form a single branch within the clan III of mammalian V region sequences in a distance tree. However, compared with a classical V gene family this branch was more diversified in sequence. Sequence analysis indicates that the apparent lack of diversity in germline V segments is well compensated for by relatively long and highly diversified D and N nucleotides. In addition, extensive sequence variation was observed in the framework region 3. Furthermore, at least five and possibly seven different J segments seem to be actively used in recombination. Interestingly, internal cysteine bridges in the complementarity-determining region (CDR)3 loop, or between the CDR2 and CDR3 loops, are found in ∼36% of the platypus VH sequences. Such cysteine bridges have also been observed in cow, camel, and shark. Internal cysteine bridges may play a role in stabilizing long and diversified CDR3 and thereby have a role in increasing the affinity of the Ab-Ag interaction.

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Evidence for an early appearance of modern post-switch isotypes in mammalian evolution; cloning of IgE, IgG and IgA from the marsupialMonodelphis domestica

Cited by 63 publications

References 44 publications

High variability in complementarity‐determining regions compensates for a low number of V gene families in the λ light chain locus of the platypus

High variability in complementarity‐determining regions compensates for a low number of V gene families in the λ light chain locus of the platypus

Mucosal Immunoglobulins

Heavy Chain V Region Diversity in the Duck-Billed Platypus (Ornithorhynchus anatinus): Long and Highly Variable Complementarity-Determining Region 3 Compensates for Limited Germline Diversity

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