Immunoglobulin D: Properties, Measurement, and Clinical Relevance

doi:10.1128/CDLI.7.2.131-140.2000

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Clinical and Diagnostic Laboratory Immunology, March 2000, p. 131-140, Vol. 7, No. 2
1071-412X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

MINIREVIEW
Immunoglobulin D: Properties, Measurement, and Clinical Relevance

Adrian O. Vladutiu^*

Departments of Pathology, Microbiology and Medicine, SUNY at Buffalo School of Medicine and Biomedical Sciences, Kaleida Health/Buffalo General Hospital, Buffalo, New York 14203

	INTRODUCTION

Top Introduction Conclusion References

Discovered in 1965 (134), immunoglobulin D (IgD) is a unique immunoglobulin with a concentration in serum far below thoseof IgG, IgA, and IgM but much higher than that of IgE. Despitestudies extending for more than 4 decades, a specific role forserum IgD has not been defined while for IgD bound to the membraneof many B lymphocytes, several functions have been proposed (15).The amount of serum IgD is measured routinely in some clinicallaboratories, almost always together with the concentrations ofIgG, IgA, and IgM, although the clinical relevance of increasedor decreased serum IgD values (in comparison to the referenceinterval or so-called normal range) has not been proven. The serendipitousdiscovery of an increased serum IgD concentration during attacksof some patients with periodic episodes of fever (156) led toa renewed search for a specific role of serum IgD. Hence, I assessedagain the clinical relevance of measuring serum IgD concentration(161). This minireview summarizes the properties of human IgDand focuses more on techniques for its measurement in serum andother body fluids and its concentration in the serum of healthyindividuals, as well as in that of subjects with various diseases.Because IgD was first found in a patient with multiple myeloma(134), monoclonal IgD is also briefly discussed. HyperimmunoglobulinemiaD syndrome (HIDS), the only entity for which the measurement ofpolyclonal IgD is necessary for diagnosis, is also very succinctlyreviewed. Recent advances focus on genes for IgD, membrane-boundIgD on B cells, signal transduction via the IgD receptor, secretionof IgD by plasma cells, and the role of IgD in T-B-cell interactions;most of the information on secreted (serum) IgD came from olderstudies.

	PROPERTIES OF IGD AND ITS ROLE IN THE IMMUNE RESPONSE

IgD represents about 0.25% of the total serum immunoglobulins and has an M_r of 185,000 and a half-life of 2.8 days (131),similar to that of IgE (162). Its synthesis rate is at least10 times lower than that of IgA, IgM, and IgG. The turnover rateis 37% of the intravascular pool per day, much higher than thatof IgG, IgA, and IgM (131) but less than that of IgE (162).The catabolism of IgD is decreased at high concentrations in serum.Initially, it was considered that about 75% of IgD was intravascular(131) but more recently it was shown in two patients with IgDmyeloma that only 31.5% of IgD was intravascular (3).

The IgD molecule has a long "hinge" region (between Fab and Fc) that appears to render the molecule very susceptible to proteolyticdegradation with production of Fab and Fc fragments (53) andalso renders the molecule flexible, thus enhancing antigen binding.The human IgD molecule has three constant-region domains. Theamino acid sequence of a monoclonal IgD was reported in 1982 (148),and the genomic sequence of human $delta$ chain was reported in 1985(167).

During storage, plasma proteases, especially plasmin, fragment the IgD molecule; the cleavage is initiated near the carboxyterminus and later in the inter-Fd-Fc area (54). The increasedsensitivity to "spontaneous" fragmentation is considered to bealso due to the Fc fragment, which is less compact for IgD thanfor other immunoglobulins (55).

IgD does not induce passive cutaneous anaphylaxis in the guinea pig (61, 118); does not bind to normal lymphocytes, neutrophils,or monocytes (80); and does not cross the placenta (84). Aggregatedmonoclonal IgD consumed C3 to C9 without loss of the early componentsof the complement cascade (63), whereas native IgD has verylittle, if any, activating activity on the components of the alternativepathway of complement (145). IgD binds bacteria nonspecificallythrough the Fc fragment; for example, it binds strongly to Neisseriacatarrhalis and Haemophilus influenzae and weakly to streptococcalgroups A, C, and G (48). IgD has antibody activity to specificantigens (34, 53, 60, 109, 110); individuals with highlevels of IgD can produce specific IgD antibodies after antigenicchallenge (62). Among 66 selected patients, 3 had IgD antibodiesto cow's milk (against bovine gamma globulin), 2 of them had antibodiesto bovine serum albumin, 1 had antibodies against diphtheria toxoid,and all 4 also had antibodies of other classes and had evidenceof vigorous immunologic responsiveness (60). Specific IgD antibodieswere also described against thyroglobulin (71), insulin in individualswith diabetes (34, 83), wheat in patients with celiac disease(6), tartrazine in certain patients with chemical hypersensitivity(165), and hepatitis B core antigen (19).

In 1972, IgD was discovered on the surface of many B cells (155); in humans and other species, IgD is the major antigen receptorisotype on the surface of most peripheral B cells, where it iscoexpressed with IgM. Few plasma cells that contain only IgD couldbe found in lymphoid tissues (136); adenoids had greater numbersof IgD-containing plasma cells than did human spleen, lymph nodes,or intestinal lymphoid tissue (122, 136). There is spontaneoussynthesis and secretion of IgD from the tonsil lymphocytes inculture (90). The heavy chains of IgD from the surface of Bcells are covalently linked by only one disulfide bridge, closeto the carboxy terminus. This allows a higher degree of freedomof the antigen-binding sites than for the other immunoglobulinisotypes (15). Serum IgD and membrane-bound IgD are antigenicallysimilar, but they differ in susceptibility to proteolysis by plasmin.Also, the $delta$ chains from membrane-bound IgD have slightly slowerelectrophoretic mobility than serum monoclonal $delta$ chains in sodiumdodecyl sulfate-polyacrylamide gel electrophoresis, suggestinga larger molecular weight for the former (146).

The signals transduced by IgM or IgD receptors on B lymphocytes are the same but with different kinetics. Signals transmittedthrough surface IgD caused induction of up to 80 different somaticmutations (95). The majority of the cell-bound IgDs are of the $kappa$ type (140), while 90% of the monoclonal IgDs in serum are ofthe $lambda$ type. The so-called IgD paradox is the preferential associationbetween $delta$ heavy chains and $lambda$ light chains in IgD-secreting cells(91). This association is expressed in vitro and in vivo, isa property of normal human IgD-secreting cells, and is closelyrelated to the secreted form of IgD. Explanations given for thepreferential association are that physical constraints favor secretory $delta$ - $lambda$ -chain association during intracellular chain assembly, IgDimmune response is highly restricted, and there is a high degreeof selectivity and unorthodox regulation of IgD light-chain expression(91). Human neoplastic B cells that expressed surface immunoglobulinsof the $lambda$ type frequently exported IgD, whereas B cells that expressedimmunoglobulins of the $kappa$ type did not export IgD (but insertedIgD into their surface membrane). This implies that possessionof a $lambda$ chain facilitates the IgD secretorypathway.

IgD production is influenced by two major factors: an independent mechanism (only for IgD), which may be genetically determined,and also the same factors that control the production of the otherimmunoglobulin isotypes (94). The genes for the C region ofµ and $delta$ (C_µ and C) are transcribed in the same RNA (acommon transcription unit) and can be expressed simultaneously.IgM and IgD molecules present on individual B cells have identicalV regions and antigen-binding sites and are coexpressed by differential(alternate) splicing of a common VDJ exon to either C_µ orC region exons to produce separate µ and $delta$ RNAs. Allelicexclusion exists for IgD, as for the other immunoglobulin classes(160). After the antigen binds to the B-cell receptor, the secretedform of $delta$ chain is shut off instead of being secreted in largeamounts, as is the case with IgM. The cells enter the pathwaysof plasma cells (which do not have IgD except for IgD-secretingplasma cells, where the µ gene is deleted) or of memory cellsin secondary lymphoid organs, cells in which IgD expression islost (12, 111). Both IgD and IgM receptors can transduce signalsby the same mechanism; however, signals mediated by engagementof surface IgD may differ from those mediated by surface IgM $---$ e.g.,only the latter cause death of cells by apoptosis (152).

After exposure to aggregated oligomeric or antigen-cross-linked monomeric secreted IgD, 10 to 15% of human peripheral bloodT cells (T $delta$ cells) exhibit receptors for IgD and form rosetteswith IgD-coated erythrocytes (26, 27). These receptors areupregulated by interleukin-2 (IL-2), IL-4, and gamma interferonon the T $delta$ cells. Both human CD4⁺ and CD8⁺ T cells can express IgD receptors (28), which can ligate membraneIgD during antigen presentation by B cells to facilitate the responsesof antigen-specific T and B cells (168).

With use of sensitive assays, IgD has been found in all of the mammalian and avian species tested and is conserved acrossspecies (89), which suggests an evolutionary advantage (15).The role of IgD (especially the secreted form) is not fully understood;it has even been thought sometime that IgD might have no function(15). This was investigated in animals treated with anti-IgDand, more recently, in IgD-deficient mice. In one model of IgDknockout mice, there was only a slight decrease in the numberof B cells in the periphery and immunoglobulin isotypes were almostnormal (112). In another model, there was a delayed affinitymaturation during T-cell-dependent antigen response (130); hence,surface-bound IgD may serve as an accelerator of affinity maturationin the primary B-cell response (125). In IgM-deficient mice,B-cell development and maturation were normal and IgD replacedmembrane-bound and secretory IgM (99). It appears that, withregard to B-cell development, IgD can largely substitute for IgMin many respects; i.e., there is redundancy between these twoisotypes (99).

Serum IgD was considered an early marker of B-cell activation (107). IgD can have a regulatory role, e.g., to enhance a protectiveantibody response of the IgM, IgG, or IgA isotype, or to interferewith viral replication (110). IgD can also participate in thegeneration and maintenance of B-cell memory and might have animportant role in the transition from a stage of susceptibilityto induction of B-cell tolerance to one of responsiveness (22,142). Finally, IgD is a potent inducer of tumor necrosis factoralpha (TNF- $alpha$ ), IL-1 $beta$ , and IL-1 receptor antagonist (38). IgDalso induces release of IL-6, IL-10, and leukemia inhibitory factorfrom peripheral blood mononuclear cells. Monocytes seem to bethe main producers of cytokines in vitro in the presence of IgD(38).

	MEASUREMENT OF IGD

The techniques used to measure IgD became more sensitive with time, and this had a bearing on the detection of low levelsof IgD, e.g., in serum of children, as well as in other body fluidsof adults. With sensitive assays, e.g., radioimmunoassay (RIA)and enzyme immunoassay (EIA), IgD was detected in the serum ofall individuals tested whereas with the less sensitive radialimmunodiffusion (RID) assay, IgD was not detected in some seraand in several other bodyfluids.

Among the techniques used to measure IgD, the first and still the most commonly used method in clinical laboratories is RID.Commercial reagents for measuring IgD by RID are readily availablefrom several companies (e.g., Beckman, Binding Site, and Behring).From an analysis of the survey (proficiency testing) for serumIgD provided by the College of American Pathologists, it appearsthat the so-called Mancini RID assay ("endpoint") technique isnow used much more often than the "timed" (Fahey and McKelvey)method (24). The former technique has a lower coefficient ofvariation (CV) than the latter. In one study, RID had a sensitivityof 10 mg/liter (68) but a significant number of individualshad undetectable amounts of serum IgD when tested with this method.Others reported 3 mg/liter as the limit of detection, but theprecision for the range between 3 and 14 mg/liter was poor (77).It is well known that gel techniques such as RID are particularlyaffected by the variability in the molecular size of the antigensbecause of alterations in the rate of diffusion through the gelwhen the size is heterogeneous (166). Therefore, IgD measurementby RID should be influenced by the high sensitivity of IgD toproteolysis, which gives rise to faster-diffusing fragments ofIgD that retain their antigenic reactivity. This means that theconcentration of IgD in old serum specimens would be overestimatedby RID, not underestimated as was recently claimed (40). Inhibitorsof proteolysis, e.g., $varepsilon$ -aminocaproic acid (final concentration,10 nM or 0.1%), aprotinin (1,000 kU/ml), or 0.01% benzamidineshould be added to serum to minimize the degradation of IgD beforemeasurement. Another disadvantage of RID is that the ring of diffusionmay pass across adjoining areas of the plate, depletes them ofantibodies, and gives incorrect results for other samples on thesame plate (166). Surprisingly, specimens stored at 37°C foreither 6 or 12 months had lost 10% of their antigenic reactivitywhen assayed by RID (137). When stored at $-$ 20°C, the rate ofIgD degradation was so low as to be negligible for 10 to 20 years(137). However, it was claimed that, despite its fragmentation,the IgD molecule could be quantitated by RID in blood stains (forforensic purposes) even after several weeks (72).

Nephelometry has also been used for IgD quantitation, but specific reagents for IgD are not readily available. From experiencegained with quantitation of other serum proteins, it appears thatthe nephelometric method is more precise, as well as more sensitive,than RID. The means of CVs obtained after the measurement by nephelometryof several serum proteins were significantly lower than the meansobtained when RID was used for measurement (126). The sensitivityof a nephelometric assay for IgD was 3 mg/liter (11). Resultsobtained with laser nephelometry apparently were not influencedby the molecular size of the protein assayed (159). Hence, thelikely fragmentation of IgD during prolonged storage is not importantfor its quantitation by nephelometry. Discrepancies between theresults obtained for the same specimens by different investigatorswith either RID or nephelometry occur when the unknown and standardsamples differ in molecular size or antigenic valence (52).It is noteworthy that in a study of 12 analytes measured by RID,electroimmunodiffusion ("rocket assay"), rate nephelometry, endpointnephelometry, immunofluorometric assay, and EIA, no method-associatedbias was observed and the results were in close agreement (126).In another experiment, a freshly drawn sample of serum was dividedinto nine aliquots and each was subjected to a different treatment(e.g., incubation at 37°C for up to 5 h and exposure to up to10 cycles of freezing and thawing). None of these treatments significantlyaltered the concentration of IgD (43).

RIA is 1,000-fold more sensitive than RID (150), and sensitivities for IgD of 10 to 50 µg/liter were reported (43, 69).After modifications, the sensitivity could be extended to 0.0008U/ml (43). When measured by RIA, IgD appears to be stable duringprolonged storage in frozen plasma; a frozen serum sample assayedrepeatedly over 2.5 years did not change in any consistent manner(44). An RIA that used paper disks had a range of measurableIgD concentrations of 2.5 to 250,000 µg/liter (8), and thesensitivity of the assay was 10 µg/liter (7). Another RIA,with the use of two antibodies, had CVs of <8% within the assayand 12% between assays (45).

EIAs for measuring serum IgD were also reported (121). Monoclonal anti-IgD antibodies were not as good as polyclonal antibodies(gave a lower optical density); and the sensitivity of the testwas 4 µg/liter (121). A sandwich EIA that utilized microtiterplates and affinity-purified goat anti-human IgD was used to reportresults as optical densities at 405 nm without the need for standards(169). Another EIA used avidin and biotin. Antibody-coated platescould be stored at 4°C for up to 1 week without loss of sensitivity,and the test showed linearity for serum dilutions of 1/200 to1/12,800. The CVs between and within assays were <10% (123).EIA and RIA have also been used to measure specific IgD (53,93, 109). Other methods used for quantitation of IgD were particlecounting immunoassay (100) and inhibition of hemagglutination(23).

As for other serum proteins, the standards (calibrators) are crucial to accurate measurement of IgD (166). Although severalreference materials are available for the three most abundantimmunoglobulins (reviewed in reference 166), there is a dearthof international reference preparations (IRP) for IgD. Internationalunits have been allocated to several international calibrantsof proteins, and collaborative efforts were undertaken to ascribemass values to them. Some of these values were "far from the truth"(166). An IRP with the declaration of a single protein, IgD,lot 67/37 (1967), has 100 U per ampoule, and the weight of lyophilizedmaterial is 81.88 mg (1-ml ampoule) (10). This is, in fact,British Research Standard 67/37, the most commonly used primarystandard (World Health Organization standard) for IgD. However,reference to the World Health Organization standard is rarelyreported and most studies have relied on a secondary referencesource. The commercially available reagents at the present timeare calibrated with a reference standard from Kallestadt (nowBeckman) or Behring. Differences between reference preparationscould be due to the freeze-drying procedure (10), which increasesthe turbidity because of an alteration in the low-density lipoproteinstructure, which is best stabilized by a high percentage of water.The use of an IgD-myeloma protein as a reference protein reducesthe reliability of the estimate (137).

The weight of IgD corresponding to 1 U of activity was calculated to be 1.41 µg. The conversion factor from grams per literto units per milliliter was obtained with the use of RID (10).This value provides only an approximate indication of the IgDcontent of a research standard. It was said that a "true value"is not near to being achieved by using grams per liter insteadof units per milliliter and that a "consensus value" (in gramsper liter) invalidates the general standardization (10). However,for many investigators, there is poor acceptance of a change inthe association from grams per liter to the abstraction of unitsper milliliter (10).

Manufacturers have to check the conversion factor from time to time and correct the value if unstable proteins have changedtheir structure. The change of a batch can cause the assignmentof a new value for the conversion factor (10). The former conversionfactor obtained by RID could no longer be confirmed, so that theIRP is not suitable in some new immunoassays. Dunnette et al.(43) found that three commercial companies had reference standardswith various ratios of mass units to units of activity (1.41,0.77, and 0.83). Yet, when their RIA for IgD measurement was comparedto the RID kits from three companies, the values obtained withthe two methods were comparable, with a CV of <16%.

The College of American Pathologists, to my knowledge, is the only organization that offers proficiency testing for serumIgD. However, of more than 3,500 laboratories that usually participatein surveys by this organization, a little more than 100 (range,>100 in 1982 to 6 in 1992) participated in the survey for IgD.According to Cheek and Papadea (24), in 1995 only 35 laboratoriesparticipated in this survey and all of the laboratories used RIDto measure serumIgD.

I reviewed the results of the surveys for IgD from 1980 to the present and noted that until 1989 the RID timed method wasused by more laboratories than the RID endpoint method. After1989, the latter method was more often used; reagents obtainedfrom only one manufacturer were used by most of the laboratories.Only one specimen is sent to laboratories for the measurementof serum IgD, in contrast to the two to four specimens sent forother determinations (e.g., for IgG). The survey specimen wassent four times per year until 1993 and thereafter only threetimes per year. The low number of laboratories that participatein the survey for IgD precludes a meaningful statistical analysisof the results. It has been noted, however, that the CV for theresults obtained by all participants in the survey for IgD thatused the RID timed method was mostly 20% or above while for theendpoint method it was slightlylower.

Some investigators (39) implied that laboratories that measure IgD in fewer than 20 specimens weekly do not have enoughvolume to maintain testing proficiency. This seems not to be thecase, since the techniques for IgD measurement are not more difficultthan similar techniques routinely used in clinical laboratoriesto measure other proteins. Also, it seems that only a very largereference laboratory, if any, measures IgD in more than 20 specimensper week, since there is not much need for thistesting.

	IGD IN BLOOD AND OTHER BODY FLUIDS OF NORMAL INDIVIDUALS

There is no single method used universally for IgD measurement, nor is there, to my knowledge, a preferred method recommendedby a professional organization or a scientific forum. Therefore,in this section, values reported for IgD were obtained with theuse of several techniques. The reported concentrations of IgDin serum and other body fluids depended on the techniques usedfor measurement when low levels of IgD were present. For example,with the use of RID, IgD was found in serum of children only afterthey had reached 12 months of age (66) and was unmeasurablein cord blood (84). In an older study, IgD was found by RIDin only 2 of 83 cord blood samples and in 4 of 90 newborn serumsamples (86). However, with use of an RIA, IgD was found incord sera of 38 of 39 newborn infants. There was no relationshipbetween the concentrations of IgD in cord blood and maternal serum,and although this suggests a fetal origin of IgD, it does notreflect the synthesis of a specific antibody but rather it maybe a developmental phenomenon (23). In newborns, the concentrationof IgD in blood was about 0.08 mg/liter (81).

The concentration of IgD in sera of infants and adults was age dependent (94) and showed considerable biological variation,even in people of the same age, from undetectable to 400 mg/liter(43, 136). Some investigators found a linear increase of IgDuntil the age of 10 (66), followed by a gradual decrease untilthe age of 14 (50). Others showed that age was not a factorin IgD levels after 6 years of age (44); indeed, there was nodifference in serum IgD concentration from 19 to 59 years of age(43). Another study also showed that the serum IgD level ofadults is attained in early childhood and persists throughoutlife (69). Levels of IgD were reported by some investigatorsto be stable in healthy adults over 1.5- and 3.5-year periods(136), but two- to threefold variations in the same individualswere seen by others when the subjects were monitored for weeksor months (81).

IgD has a remarkably wide normal range in serum, probably because of striking differences in its rate of synthesis (131).A study of 200 sera showed that the range was wider (4 logs) thanfor any other immunoglobulin (150). The median concentrationof serum IgD was 30 mg/liter when determined by RID (135). Theserum IgD levels (measured by RIA) for 85 normal adults rangedbetween 0.2 and 121 mg/liter, with an arithmetic mean of 25 mg/liter(17.7 U/ml) (45) and apparently had a trimodal distribution,with modes at about 0.25, 5.1, and 35 U/ml (43). Others couldnot find a trimodal distribution (69). Many reference intervals("normal ranges") for IgD concentration in serum have been reported,e.g., 14 to 85 mg/liter (144), 10 to 112 mg/liter (21), and5 to 240 mg/liter (97). Averages were also scattered, e.g.,50 mg/liter (77), 40 mg/liter (76), 35 mg/liter (97), and25 mg/liter (45). Since the values for serum IgD did not followa Gaussian distribution (43), it was common to transform theresults into square roots (78) or a natural logarithmic scalefor statistical analysis (78, 114, 121).

Individuals can be high or low producers of (serum) IgD (94). Early studies have suggested that about 10 to 14% of individualshad very low concentrations of serum IgD, i.e., <3 mg/liter (43,81) and that about 10% have high concentrations (>100 mg/liter).It was hypothesized, but not proven (94), that low producerscan convert to high producers because of infections and immuneactivation. Low serum IgD was not dependent on age and was notrelated to sex (44). It has also been suggested that the lowIgD level is genetically determined, with autosomal recessiveinheritance (44). However, low serum IgD was seen in 44% ofchildren of parents with high IgD, making autosomal inheritanceunlikely (44). No inheritance pattern was observed for highlevels of IgD (44). Dunnette et al. (43) proposed, on thebasis of mathematical analysis (Hardy-Weinberg equation), thatlevels of IgD in normal individuals are strongly influenced byinheritance through a monogenic mechanism. Twin studies also supportedan influence of inheritance on the serum IgD concentration (1,81) but there are also environmental influences (100). It wasreported that Gm allotype (163) and histocompatibility antigens(44, 49) can influence IgDlevels.

There was a positive correlation among serum IgD concentration, the number of IgD-positive plasma cells in bone marrow (62),and spontaneous in vitro IgD secretion by B lymphocytes (92).However, there was no correlation between the amount of IgD inserum and the amount expressed by lymphocytes (69). A positivecorrelation was found between serum IgD level and serum IgA andIgE levels (69), white blood cell count, and number of CD4⁺ and CD25⁺ lymphocytes but not with other immunoglobulin isotypes or markersof immune activation (94). Although the amount of IgD usuallyparalleled the amount of other immunoglobulins in serum (45),the values of IgG and IgM did not always correlate with the presenceor absence of IgD, as detected by double-diffusion-in-gel assay(120).

It has been proposed that the female sex hormone influences IgD synthesis (76), although values for serum IgD in males andfemales were similar in many studies (43, 44, 135). In anotherstudy, females 1 through 5 years of age had higher serum IgD concentrationsthan males (86). The concentration of IgD was also elevatedin pregnant women (76) and increased throughout gestation (85),also suggesting that hormonal factors influence IgD metabolism(76). A highly significant exponential correlation was reportedbetween maternal IgD levels and gestational age (78). IgD wasalso elevated in maternal sera at term, but the influence of labor(76, 85) and delivery was not clear (58, 76, 85). IncreasedIgD levels in maternal sera at term may represent antibodies directedto either leukocytes or trophoblastic antigens (76). HLA-A2and HLA-A13 in the mother was correlated with IgD concentrationat delivery (78). Sera of women with premature delivery hada significantly lower mean concentration of IgD than other groups(78). A correlation between parity and IgD level was also reported(85).

IgD was not detected by RID in 10-fold-concentrated saliva, bile, highly concentrated urine, concentrated tears, and unconcentratedcerebrospinal fluid (136). Isoelectric focusing of unconcentratedcerebrospinal fluid showed oligoclonal and polyclonal IgD patterns(102). Human colostrum (8) and milk contain considerable quantitiesof IgD (43, 93); IgD was found in all 11 specimens of milktested, with an arithmetic mean of 1,150 U/liter, a geometricmean of 161 U/liter, and a median of 137 U/liter (range, 8 to8,600 U/liter) (43). Values of IgD in nasal washings rangedfrom 11 to 503 U/g of protein; the values were higher than insaliva (123).

	SERUM IGD IN VARIOUS DISEASES AND CONDITIONS

The meaning of an abnormal (increased or decreased) concentration of serum IgD is not known. An increase in serum IgD doesnot imply the generation of antibodies of the IgD class in eachindividual (62).

IgD was measured in the sera of subjects with various conditions, and although the values obtained probably depended somewhaton the techniques used for measurement, the results from patientswith various diseases were compared to findings obtained by thesame techniques from healthy individuals, so the conclusions werevalid. As just mentioned, the most important factor for the accuracyof IgD measurement is the standard used in the assays. The sensitivityof the techniques is less important when testing various patientsfor increased or decreased serum IgD values (in comparison tohealthy subjects). A technique with low sensitivity might notdetect very low levels of IgD in some patients, but this has noclinical importance. There have not been, to my knowledge (norwere any expected), reports of increased sensitivity of IgD toproteolytic enzymes in patients with certain diseases. Althoughthe storage of specimens for IgD quantitation is of some importancewhen RID is used to measure IgD, this is not likely to introducebias in the values of IgD found in patients with various diseasesor conditions compared to healthy individuals if the storage wassimilar for all specimens. Many individuals with high levels ofone or more immunoglobulin isotypes have low or normal levelsof IgD, and occasionally normal or high values for serum IgD wereseen in hypogammaglobulinemic patients (21, 136, 161). Ina study of 58 patients with IgG paraproteinemia, of whom 34 hadmultiple myeloma, a negative correlation for IgD was found (151),and in 133 patients with monoclonal gammopathies, IgD concentrationdecreased in parallel with polyclonal immunoglobulin levels (46).Hiemstra et al. (62) studied 17 patients with high serum IgDlevels (250 to 5,311 U/ml), both children and adults, and concludedthat there was no apparent relationship between several clinicalsyndromes and the increased serum IgD. In many studies of patientswith various diseases, only serum IgD levels were reported whereasin some patients with certain diseases or conditions (e.g., atopy)the amounts of other immunoglobulins were reported as well. Becausethis minireview is focused on IgD, the serum levels of other immunoglobulinsmeasured in conjunction with IgD are notgiven.

Infections. IgD antibody seemed to behave like IgM antibody at the early stage of infection (149). There was a significant positive correlationbetween the levels of IgD and the titers of complement-fixingantibody to Mycobacterium pneumoniae (149). Specific IgD antibodieswere also found in patients with rubella (139), and IgD antibodiesto measles virus were found in patients with subacute sclerosingpanencephalitis (96). IgD antibodies to diphtheria toxin, Escherichiacoli, and streptolysin O were also reported (60, 67, 143,147). A 22-year-old female with presumed coxsackievirus myocarditishad an increased serum IgD level (4).

Chronic infections were also considered to raise the concentrations of serum IgD (136); indeed, serum IgD was increased inpatients with leprosy (144), tuberculosis (20, 74), salmonellosis,infectious hepatitis (133), and malaria (29). In a 7-year-oldchild with a history of recurrent infections, a high level ofIgD was noted in serum (125). Many, but not all, patients withelevated IgD (measured by RID) had recurrent staphylococcal infections(21), and increased values of serum IgD were found in some patientswith viral infections (132, 139). The clinical relevance ofall of these specific IgD antibodies, if any, is notknown.

Immunodeficiencies. Patients with immunodeficiencies very often have various infections; hence, it is unclear whether IgD concentrations in thesepatients reflect immunodeficiency itself or infections. Thereis no uniform pattern of IgD production in defined primary immunodeficiencies;some individuals had increased levels, and some had decreasedlevels (94). Within the whole group of immunodeficiencies, apositive correlation of IgD with IgA and IgE was noted. A positivecorrelation of serum IgA and IgD levels was also found in humanimmunodeficiency virus-infected patients (108). With an RID assay,IgD was detected in serum in only 49% of IgA-deficient patients(21) and numerous IgD-producing plasma cells were found in thelacrimal and parotid glands, suggesting that secretory IgD playsa compensatory role in IgA deficiency (17). Some patients withhyper-IgE syndrome, who often have recurrent infections with staphylococcus,had high serum IgD levels, but the cause for this is not known(69). Low levels of IgD in the hyper-IgE syndrome were alsoreported (42). Group mean concentrations of IgD in plasma weredepressed in patients with Wiscott-Aldrich syndrome (21). Inthree children with agammaglobulinemia (no B cells in the blood),the serum IgD level was higher than in healthy children (21).IgD was increased in plasma of patients with Nezelof syndrome(21) and in children with ataxia telangiectasia (105). A highserum IgD value was found in a girl with immunodeficiency andincreased serum IgM (9). Serum IgD was increased in patientswith impaired cell-mediated immunity, e.g., those with allergicbronchopulmonary aspergillosis (97) and sarcoidosis (20),as well as in patients with AIDS (25, 107, 108, 120). Recently,it was shown in 131 children with many types of immunodeficiencies(including CD40 ligand [CD 145] deficiency) that the serum IgDlevel was not of particular value in the investigation of immunodeficientchildren; the serum IgD level was not associated with the generalpicture of immune activation (94).

Autoimmune and allergic diseases. Serum IgD was increased in patients with autoimmune diseases who also had increased IgG, IgA, and IgM (83, 87, 116, 133,141). High values of serum IgD were found in some, but not all,adults with rheumatoid arthritis (136) and in children with juvenilerheumatoid arthritis (51). Antinuclear antibodies of the IgDclass were found in patients with systemic lupus erythematosus(53, 98, 128, 164), and a slight increase of serum IgD wasfound in patients with Sjögren's syndrome and in a patient withautoimmune thyroiditis (71). Autoantibodies of the IgD classwere found in some patients with scleroderma (98) and atopicdiseases (74, 77, 97, 169), e.g., atopic dermatitis (18,69). IgD was reported to be increased or decreased in sera ofpatients with allergic asthma (74, 77, 97), but a considerableoverlap existed between healthy and allergic subjects. In theatopic group, the mean serum IgD level did not differ significantlyon the basis of age, sex, or asthmatic status (121). In patientswith asthma, basophil degranulation by a high anti-IgD concentrationwas reported (121).

IgD against birch and timothy pollen allergens was increased in sera of atopics with IgE antibodies to birch pollen allergens,compared to sera of atopics without IgE against these allergens.The allergen specificity of IgD antibodies was confirmed withan allergen inhibition test. However, no significant correlationwas found between total serum IgD and IgE (169). IgD antibodiesspecific for a benzylpenicilloyl epitope were found in some patientswith penicillin allergy (53), and IgD was also found on redcells from patients with hemolytic anemia caused by penicillin(88), but the clinical value of these antibodies isdoubtful.

Other conditions. The geometric mean of the IgD concentrations in sera of cigarette smokers was twice as high as in nonsmokers. In the smokinggroup, it was the highest in those who did not actively inhalesmoke (fourfold higher than in nonsmokers) and the lowest in heavysmokers who inhaled (8). The IgD level was more strongly relatedto the number of cigarettes smoked per day than to the years ofsmoking. Cessation of smoking was followed by normalization ofthe IgD level (8). The influence of maternal smoking was moreevident in newborns of nonallergic parents; even paternal smokingincreased the level of cord serum IgD in these newborns (100).The reason for the increased IgD in smokers is not known; it couldbe because of infections. B cells may be stimulated by mild tomoderate degrees of smoking but suppressed by heavy smoking (8),and it is likely that the influence of substances in tobacco smokeis not directly on B cells but on regulatory Tcells.

A definite increase in serum IgD was found in patients with Hodgkin's disease several months after splenectomy (31). A correlationwith the histologic type was observed; e.g., patients in the lymphocyte-depletedgroup had extremely high levels of IgD (log mean, 284 mg/liter).Also, patients who received treatment had significantly lowervalues than untreated patients (30, 31) and there was a definitetendency toward lower levels in older patients (31). A fallin serum IgD was seen after radiotherapy but not after chemotherapyin patients with lymphoma (2). When RID was used to measureIgD, the values fell in stages III and IV; IgD was not detectablein 30% of patients with lymphoma (but also in 39% of healthy controls)(2).

Increased concentrations of serum IgD were found in other diseases and conditions, e.g., in children with kwashiorkor (136),(transiently) after allogeneic bone marrow transplantation (107);very rarely in patients with Behçet syndrome; and in those withidiopathic retinal vasculitis (79). In this latter condition,a linear correlation was found between serum IgD levels and thepercentage of IgD-positive B cells in the blood (79). The geometricmean of IgD concentrations in the sera of nine children with Henöch-Schoenleinpurpura was significantly higher than that in sera of controlchildren (16.7 versus 9.1 mg/liter); increased IgD levels werefound only in children who did not have nephritis (140). Thegeometric mean of serum IgD values was significantly higher inpatients with chronic obstructive pulmonary disease than in healthyindividuals (106). However, the distribution of IgD in each groupshowed marked positive skewedness (114). High values of serumIgD were also found in children following chemotherapy for malignancies(5) and in some patients with hyperparathyroidism (120). Insome patients with central nervous system tumors, increased serumIgD levels, as well as oligoclonal bands of IgD in spinal fluid(103), suggested that systemic IgD production in these patientsoccurred independently of IgG (104). High IgD values (comparedto those of healthy individuals) were reported in the sera offour patients with aortitis (116) and in a few patients withliver cirrhosis (116).

Monoclonal IgD. The measurement of serum IgD is most important for the monitoring (and the diagnosis) of IgD gammopathies (IgD myeloma and $delta$ heavy-chain disease). IgD myeloma represented 1.8% (154) and1.2% (65) of multiple myelomas in two series. It has an aggressivecourse, often with extramedullary involvement, amyloidosis, lymphadenopathy,splenomegaly, severe anemia, azotemia, very often ( $>=$ 90%) BenceJones proteinuria (14, 47), and short survival (82). M components(with $gamma$ -, $beta$ -, or $alpha$ ₂-globulin mobility), representing monoclonalIgD, were seen in only 60% of the serum protein electrophoresesof patients with IgD myeloma (14); the remaining patients hadnormal electrophoresis or hypogammaglobulinemia (14, 47).The range of monoclonal IgD concentrations in serum was 800 to66,000 mg/liter (65). From 60% (14) to 90% (65) of IgD myelomasare of the $lambda$ type. The rarity of IgD $kappa$ secretion was explainedby a block in the assembly, glycosylation, and secretion of thisimmunoglobulin or rapid intracellular catabolism of IgD $kappa$ destinedfor secretion (70). There is antigenic heterogeneity among monoclonalIgDs (probably allotypic variants, not subclasses, of IgD) (115,129). A patient with IgD myeloma had separate heavy- and light-chainM components in the serum, probably because of an intracellularassembly defect (158). A monoclonal IgD had antibody activityagainst triglycerides, and the patient had hyperlipidemia (127).Another monoclonal IgD $lambda$ had pyroglobulin activity (precipitatedirreversibly at 56°C) (153). Finally, an increased serum viscosityof 6.8 U (reference, <1.8 U) was reported for a monoclonal IgD(117). Only three patients with monoclonal IgD of undeterminedsignificance were reported (13, 75, 113). The only patientwith $delta$ heavy-chain disease reported so far was a 70-year-old malewho presented with symptoms of multiple myeloma and died withkidney complications (157).

HIDS. The new syndrome HIDS (MIM 260920) (so named in 1995) was described in 1984 by Van der Meer et al. (156) and seems to haveboosted the measurement of serum IgD in various patients in thehope of detecting more patients with HIDS and also of findingincreased IgD in other conditions. In 1983, Prieur and Griscellidescribed eight patients with juvenile onset of periodic feverand joint disease who were later shown to have increased serumIgD, as seen in HIDS (124). Originally described in patientsfrom Holland, HIDS was found mostly in European countries (32)and later also in the United States (56). HIDS was found inpatients with periodic fever that resembles familial Mediterraneanfever (MIM 249100) and chronic, infantile, neurological, cutaneous,and articular syndrome. To my knowledge, 144 cases have been recordedin the international registry by the end of 1999. This syndromeis characterized by recurrent febrile attacks accompanied by abdominalpain, arthralgia, headache, and skin lesions. In the first reportedcases of HIDS, IgD was measured by RID in specimens of serum towhich $varepsilon$ -aminocaproic acid was added to inhibit proteolysis. Skinmanifestations occurred in 80% of patients with HIDS but did notcorrelate with the serum IgD levels (57). During the febrileepisodes, all patients had serum IgD values above 60 mg/liter(35) or 100 U/ml measured, if possible, on two occasions atleast 1 month apart (36). Between attacks, IgD was as low as11, 15.1, and 39 U/liter in three patients but rose to 656, 1,743,and 600 U/liter, respectively, during attacks (36). In two patients,the clinical symptoms of HIDS preceded the rise in serum IgD,indicating that elevated IgD concentration is not the cause ofthe clinical symptoms in this syndrome (59).

HIDS is probably inherited as an autosomal recessive trait (33). Very recently, mutations in the mevalonate kinase genewere shown to cause HIDS (41, 64). It has been proposed thatpatients exhibit an uncontrolled type III hypersensitivity reaction,possibly with involvement of IgD-containing complexes (16).Complement deficiencies or decreases in serum C3 and C4 were notfound, albeit circulating immune complexes were detected in 20%of patients during or between attacks (36). A linear correlationwas observed between serum IgD level and serum IgD complexes (62).During the febrile episodes, inflammatory cytokines, e.g., IL-6,TNF- $alpha$ , and gamma interferon, were increased together with naturallyoccurring inhibitors such as IL-1 receptor antagonist and solubleTNF receptor (37). It was suggested that the underlying disturbancesin HIDS may be in the T-cell regulation resulting in abnormalproduction of IgD primarily of the $kappa$ type, as well as of IgA,IgM, and IgG3 (59).

IgD was also increased (>100 U/ml) in many children with periodic fever, aphthous stomatitis, pharyngitis, and adenopathysyndrome (119), which was described in 1987 by Marshall et al.(101). This syndrome differs from HIDS and is self-limited (HIDScan persist throughout life) and responds dramatically to a singleoral dose of corticosteroids (119).

	CONCLUDING REMARKS

Top Introduction Conclusion References

Although considerably more is known now about IgD than several decades ago soon after it was discovered, most of the recentinformation pertains to membrane-bound, not to serum, IgD. Recently,renewed interest in serum IgD measurement came from the chancediscovery that some children with periodic fever had increasedlevels of serum IgD during the attacks (156). Increased serumIgD was found in many conditions but not always with consistencyand has no practical value. A decreased level of serum IgD alsohas no clinical value. Serum IgD measurement can be importantfor monitoring of IgD myelomas, and it has been recently restatedthat monoclonal immunoglobulins are more accurately quantitatedby measuring the protein concentration of the M spike in serumprotein electrophoresis than by measuring the specific monoclonalimmunoglobulin (73). The former procedure could be more difficultto perform for IgD because it migrates faster than IgG in serumprotein electrophoresis, often together with other beta globulins,and sometimes the homogeneous IgD band is faint (154). The increasedsensitivity of IgD to proteolysis could give false elevated levelswhen IgD is measured by RID in specimens that were not properlystored and to which protease inhibitors were not added. Expressionof results in international units versus mass units (milligramsper liter) remains debatable, especially since no new IRP of IgDis available. To measure serum IgD in many patients only for thepurpose of retaining competency (39) is unwarranted becausemeasurement of IgD is not technically different from or more demandingthan other routine measurements, and no clinical value of a findingof increased or decreased serum IgD has been shown. The possibilityof finding a disease or another syndrome always associated withhigh serum IgD is very remote and likely of no clinical relevance.From experience, it seems that a specific role for serum IgD willnot be found in the near future. In the present climate of costcontainment in clinical laboratories, it is not justifiable tocontinue routinely measuring IgD every time other immunoglobulins(e.g., IgG, IgA, and IgM) are quantitated, or even separately,except in the cases of patients with monoclonal IgD in the serumor patients suspected of havingHIDS.

	ACKNOWLEDGMENTS

I thank R. Tomar, H. Spiegelberg, and D. Rappette for helpful information and J. Teitz for preparing themanuscript.

	FOOTNOTES

^* Mailing address: Department of Pathology, Immunopathology Laboratory, Kaleida Health/Buffalo General Hospital, 100 High St.,Buffalo, NY 14203. Phone: (716) 859-2509. Fax: (716) 859-2393.E-mail: vladutiu{at}acsu.buffalo.edu.

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72. Keil, W., and M.-L. Glowatzki. 1986. Quantitative IgD measurement for discrimination of human blood stains. Forensic Sci. Int. 31:73-78[CrossRef][Medline].

73. Keren, D. F., R. Alexanian, J. A. Golken, P. D. Gorevic, R. A. Kyle, and R. H. Tomar. 1999. Guidelines for clinical laboratory evaluation of patients with monoclonal gammopathies. Arch. Pathol. Lab. Med. 123:106-107[Medline].

74. Kikindjanin, V. 1981. IgD value in children suffering from acute, recurrent and chronic respiratory diseases. Allerg. Immunol. 27:203-206.

75. Kinoshita, T., H. Nagai, T. Murate, H. Saito, T. Fukatsu, and T. Hotta. 1997. IgD monoclonal gammopathy of undetermined significance. Int. J. Hematol. 65:169-172[CrossRef][Medline].

76. Klapper, D. G., and H. W. Mendenhall. 1971. Immunoglobulin D concentrations in pregnant women. J. Immunol. 107:912-915[Abstract/Free Full Text].

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78. Kretschmer, R. R., H. Gomez-Estrada, J. C. Margain, J. Arellano, R. Ramos, and P. Landazuri. 1975. Serum IgD concentration in pregnant women. Clin. Immunol. Immunopathol. 4:9-15[CrossRef][Medline].

79. Kumano, Y., T. Nagato, K. Kurihara, H. Kikukawa, M. Goto, Y. Kawano, Y. Ohnishi, and H. Inomata. 1997. Hyperimmunoglobulinemia D in idiopathic retinal vasculitis. Graefes Arch. Clin. Exp. Ophthalmol. 235:372-378[CrossRef][Medline].

80. Lawrence, D. A., W. O. Weigle, and H. L. Spiegelberg. 1975. Immunoglobulins cytophilic for human lymphocytes, monocytes and neutrophils. J. Clin. Investig. 55:368-387.

81. Lee, S. K., J. D. Metrakos, K. R. Tanaka, and D. C. Heiner. 1980. Genetic influence on serum IgD levels. Pediatr. Res. 14:60-63[Medline].

82. Le Quellec, A., R. Bataille, M. Levy-Robinet, J. Santy, and A. J. Ciurana. 1989. Myèlome multiple à immunoglobuline D. Etude rétrospective dans le Languedoc. Presse Med. 18:1110-1113.

83. Lertora, J. J. L., F. J. Gomez-Perez, and G. A. Leslie. 1975. Structure and biological functions of human IgD. V. Insulin antibodies of the IgD class in sera from some diabetic patients. Int. Arch. Allergy Appl. Immunol. 49:597-606[Medline].

84. Leslie, G. A., and T. E. Swate. 1972. Structure and biological function of human IgD. 1. The presence of IgD in human cord sera. J. Immunol. 109:47-50[Abstract/Free Full Text].

85. Leslie, A., and R. C. Armen. 1975. Structure and biologic functions of human IgD. II. Alteration of serum IgD levels during pregnancy. Proc. Soc. Exp. Biol. Med. 144:741-743[Medline].

86. Leslie, G. A., R. H. Lopez-Correra, and J. N. Holmes. 1975. Structure and biological functions of human IgD. IV. Ontogeny of human serum immunoglobulin D (IgD) as related to IgG, IgA and IgM. Int. Arch. Allergy Appl. Immunol. 49:350-357[Medline].

87. Leslie, G. A., and L. N. Martin. 1978. Structure and function of serum and membrane immunoglobulin D (IgD). Contemp. Top. Mol. Immunol. 7:1-49[Medline].

88. Levine, B. B., and A. Redmond. 1967. Immunochemical mechanisms of penicillin induced Coombs positivity and hemolytic anemia in man. Int. Arch. Allergy Appl. Immunol. 31:594-606[Medline].

89. Lin, L. C., and F. W. Putnam. 1981. Primary structure of the Fc region of human IgD: implications of evolutionary origin and biologic function. Proc. Natl. Acad. Sci. USA 78:504-508[Abstract/Free Full Text].

90. Litwin, S. D., and B. D. Zehr. 1987. In vitro studies on human IgD. I. Sources and characteristics of "externalized" IgD in tonsil lymphocyte cultures. Eur. J. Immunol. 17:483-489[Medline].

91. Litwin, S. D., and B. D. Zehr. 1987. In vitro studies on human IgD. II. IgD-secreting cells preferentially elaborate IgD, $lambda$ molecules. Eur. J. Immunol. 17:491-495[Medline].

92. Litwin, S. D., and B. D. Zehr. 1988. In vitro studies on human IgD and spontaneous IgD biosynthesis. Clin. Immunol. Immunopathol. 47:75-83[CrossRef][Medline].

93. Litwin, S. D., B. D. Zehr, and R. A. Insel. 1990. Selective concentration of IgD class-specific antibodies in human milk. Clin. Exp. Immunol. 80:263-267[Medline].

94. Litzman, J., A. M. Ward, G. Wild, V. Znojil, and G. Morgan. 1997. Serum IgD levels in children under investigation for and with defined immunodeficiency. Int. Arch. Allergy Immunol. 114:54-58[CrossRef][Medline].

95. Liu, Y.-J., O. de Bouteiller, C. Arpin, F. Briere, L. Galibert, S. Ho, H. Martinez-Valdez, J. Banchereau, and S. Lebecque. 1996. Normal human IgD⁺/IgM⁺ germinal center B cells can express up to 80 mutations in the variable region of their IgD transcripts. Immunity 4:603-613[CrossRef][Medline].

96. Luster, M. I., R. C. Armen, J. V. Hallum, and G. A. Leslie. 1976. Measles virus-specific antibodies in patients with subacute sclerosing panencephalitis. Proc. Natl. Acad. Sci. USA 73:1297-1299[Abstract/Free Full Text].

97. Luster, M. I., G. A. Leslie, and E. J. Bardana, Jr. 1976. Structure and biological function of human IgD. VI. Serum IgD in patients with allergic bronchopulmonary aspergillosis. Int. Arch. Allergy Appl. Immunol. 50:212-219[Medline].

98. Luster, M. I., G. A. Leslie, and E. J. Bardana, Jr. 1976. Structure and biological functions of human IgD. VII. IgD antinuclear antibodies in sera of patients with autoimmune disorders. Int. Arch. Allergy Appl. Immunol. 52:212-218[Medline].

99. Lutz, C., B. Ledermann, M. H. Kosco-Vilbois, G. Kohler, and F. Brombacher. 1998. IgD can largely substitute for loss of IgM function in B cells. Nature 393:797-801

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MINIREVIEW Immunoglobulin D: Properties, Measurement, and Clinical Relevance

MINIREVIEW
Immunoglobulin D: Properties, Measurement, and Clinical Relevance