Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:5.99.1.2 (
topoisomerase
)
9,166
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Activation-induced cytidine deaminase
(
AID
) is essential and sufficient to accomplish class-switch recombination and somatic hypermutation, which are two genetic events required for the generation of antibody-mediated memory responses. However,
AID
can also introduce genomic instability, giving rise to chromosomal translocation and/or mutations in proto-oncogenes. It is therefore important for cells to suppress
AID
expression unless B lymphocytes are stimulated by pathogens. The mechanisms for avoiding the accidental activation of
AID
and thereby avoiding genomic instability can be classified into three types: (i) transcriptional regulation, (ii) post-transcriptional regulation and (iii) target specificity. This review summarizes the recently elucidated comprehensive transcriptional regulation mechanisms of the
AID
gene and the post-transcriptional regulation that may be critical for preventing excess
AID
activity. Finally, we discuss why
AID
targets not only Igs but also other proto-oncogenes.
AID
targets many genes but it is not totally promiscuous and the criteria that specify its targets are unclear. A recent finding that a non-B DNA structure forms upon a decrease in
topoisomerase
1 expression may explain this paradoxical target specificity determination. Evolution has chosen
AID
as a mutator of Ig genes because of its efficient DNA cleavage activity, even though its presence increases the risk of genomic instability. This is probably because immediate protection against pathogens is more critical for species survival than complete protection from the slower acting consequences of genomic instability, such as tumor formation.
...
PMID:Preventing AID, a physiological mutator, from deleterious activation: regulation of the genomic instability that is associated with antibody diversity. 2020 15
Activation-induced cytidine deaminase
(
AID
), which is both essential and sufficient for forming antibody memory, is also linked to tumorigenesis.
AID
is found in many B lymphomas, in myeloid leukemia, and in pathogen-induced tumors such as adult T cell leukemia. Although there is no solid evidence that
AID
causes human tumors,
AID
-transgenic and
AID
-deficient mouse models indicate that
AID
is both sufficient and required for tumorigenesis. Recently,
AID
's ability to cleave DNA has been shown to depend on
topoisomerase
1 (Top1) and a histone H3K4 epigenetic mark. When the level of Top1 protein is decreased by
AID
activation, it induces irreversible cleavage in highly transcribed targets. This finding and others led to the idea that there is an evolutionary link between meiotic recombination and class switch recombination, which share H3K4 trimethyl,
topoisomerase
, the MRN complex, mismatch repair family proteins, and exonuclease 3. As Top1 has recently been shown to be involved in many transcription-associated genome instabilities, it is likely that
AID
took advantage of basic genome instability or diversification to evolve its mechanism for immune diversity.
AID
targets are therefore not highly specific to immunoglobulin genes and are relatively abundant, although they have strict requirements for transcription-induced H3K4 trimethyl modification and repetitive sequences prone to forming non-B structures. Inevitably,
AID
-dependent cleavage takes place in nonimmunoglobulin targets and eventually causes tumors. However, battles against infection are waged in the context of acute emergencies, while tumorigenesis is rather a chronic, long-term process. In the interest of survival, vertebrates must have evolved
AID
to prevent infection despite its long-term risk of causing tumorigenesis.
...
PMID:The AID dilemma: infection, or cancer? 2242 51
