Immunoglobulin M (IgM) is an antibody produced by B cells. IgM is by far the physically largest antibody in the human circulatory system. It is the first antibody to appear in response to initial exposure to an antigen.^[1][2] The spleen, where plasmablasts responsible for antibody production reside, is the major site of specific IgM production.^[3][4]

Structure and function

IgM is a polymer, where multiple immunoglobulins are linked together by strong covalent bonds known as disulfide bonds. IgM exists most commonly as a pentamer (5 linked immunoglobulins) but also as a hexamer (six linked immunoglobulins). IgM has a molecular mass of approximately 970 kDa (in its pentamer form).^[5] Because each immunoglobulin monomer has two antigen binding sites, a pentameric IgM has 10 binding sites. Typically, however, IgM cannot bind 10 antigens at the same time because the large size of most antigens hinders binding to nearby sites.

The J chain of the antibody is found in pentameric IgM but not in the hexameric form, perhaps due to space constraints in the hexameric complex. Pentameric IgM can also be made in the absence of J chain. At present, it is still uncertain what fraction of normal pentamer contains J chain, and to this extent it is also uncertain whether a J chain-containing pentamer contains one or more than one J chain.^[6] Although hexameric IgM without J chain has higher efficiency of complement fixation than pentameric IgM with J chain.^[6][7]

Because IgM is a large molecule, it cannot diffuse well, and is found in the interstitium only in very low quantities. IgM is primarily found in serum; however, because of the J chain, it is also important as a secretory immunoglobulin.^[8]

Due to its polymeric nature, IgM possesses high avidity, and is particularly effective at complement activation. By itself, IgM is an ineffective opsonin; however it contributes greatly to opsonization by activating complement and causing C3b to bind to the antigen.^[9]

Expression

In germline cells, the gene segment encoding the μ constant region of the heavy chain is positioned first among other constant region gene segments. For this reason, IgM is the first immunoglobulin expressed by mature B cells.

On mature B cells, both IgM and IgD are co-expressed through long mRNA transcripts which undergo differential splicing; the transcript for IgM is produced when the VDJ exon is spliced to the Cμ exon, with polyadenylation at p(A1).^[10] In contrast the IgD transcript is produced when the VDJ exon is spliced to Cδ exons, with polyadenylation further downstream at p(A2).^[10]

It is also the first immunoglobulin expressed in the fetus (around 20 weeks)^[11] and phylogenetically the earliest antibody to develop.^[12]

Clinical significance

IgM antibodies appear early in the course of an infection and usually reappear, to a lesser extent, after further exposure. IgM antibodies do not pass across the human placenta (only isotype IgG).

These two biological properties of IgM make it useful in the diagnosis of infectious diseases. Demonstrating IgM antibodies in a patient's serum indicates recent infection, or in a neonate's serum indicates intrauterine infection (e.g. congenital rubella syndrome).

The development of anti-donor IgM after organ transplantation is not associated with graft rejection but it may have a protective effect.^[13]

Research applications

In research, purified antibodies are used in many applications. IgM antibodies for research applications can be found directly from antibody suppliers, or through use of specialist search engines like CiteAb, Antibodypedia, and SeekProducts. Research antibodies are most commonly used to identify and locate intracellular and extracellular proteins.

Researchers using antibodies in their work need to record them correctly in order to allow their research to be reproducible (and therefore tested, and qualified by other researchers). Less than half of research antibodies referenced in academic papers can be easily identified.^[14] A paper published in F1000 in 2014 provided researchers with a guide for reporting research antibody use.^[15]

Other points

IgM in normal serum is often found to bind to specific antigens, even in the absence of prior immunization.^[16] For this reason IgM has sometimes been called a "natural antibody". This phenomenon is probably due to the high avidity of IgM that allow it to bind detectably even to weakly cross-reacting antigens that are naturally occurring. For example, the IgM antibodies that bind to the red blood cell A and B antigens might be formed in early life as a result of exposure to A- and B-like substances that are present on bacteria or perhaps also on plant materials.

IgM antibodies are mainly responsible for the clumping (agglutination) of red blood cells if the recipient of a blood transfusion receives blood that is not compatible with their blood type.

IgM is more sensitive to denaturation by 2-mercaptoethanol than IgG.^[17] This technique was historically used to distinguish between these isotypes before specific anti-IgG and anti-IgM secondary antibodies for immunoassays became commercially available. Serum samples would be tested for reactivity with an antigen before or after 2-mercaptoethanol treatment to determine whether the activity was due to IgM or IgG.^[17][18]

See also

• Immunodeficiency with hyper-immunoglobulin M
• Immunoglobulin M deficiency

References

External links

• Immunoglobulin M at the US National Library of Medicine Medical Subject Headings (MeSH)
• Immunoglobulin M Deficiency Reference from Medscape.com