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Factors associated with IgG levels in adults with IgG subclass deficiency

BMC Immunology volume 22, Article number: 53 (2021) Cite this article

Abstract

Background

Factors associated with IgG levels in adults with IgG subclass deficiency (IgGSD) are incompletely understood. We studied adults with IgGSD with subnormal IgG1 only, subnormal IgG1/IgG3, or subnormal IgG3 only without other subnormal IgG subclasses, IgA, or IgM. We compiled: age; sex; autoimmune condition(s) (AC); atopy; IgG, IgG subclasses, IgA, IgM; IgGsum (IgG1 + IgG2 + IgG3 + IgG4); and D (percentage difference between IgGsum and IgG). We compared attributes of patients with/without subnormal IgG (< 7.00 g/L; subnormal IgG1 subclass groups only) and analyzed IgGsum and IgG relationships. We performed backward stepwise regressions on IgG using independent variables IgG subclasses, age, and sex and on D using independent variables age and sex.

Results

There were 39 patients with subnormal IgG1 only (89.7% women), 53 with subnormal IgG1/IgG3 (88.7% women), and 115 with subnormal IgG3 only (91.3% women). Fifteen patients (38.5%) and 32 patients (60.4%) in the respective subnormal IgG1 subclass groups had subnormal IgG. Attributes of patients with/without IgG < 7.00 g/L were similar, except that AC prevalence was lower in patients with subnormal IgG1 only and IgG < 7.00 g/L than ≥ 7.00 g/L (p = 0.0484). Mean/median IgG1 and IgG2 were significantly lower in patients with IgG < 7.00 g/L in both subnormal IgG1 subclass groups (p < 0.0001, all comparisons). Regressions on IgG in three subclass groups revealed positive associations with IgG1 and IgG2 (p < 0.0001 each association). Regressions on D revealed no significant association. IgG1 percentages of IgGsum were lower and IgG2 percentages were higher in patients with subnormal IgG1 subclass levels than subnormal IgG3 only (p < 0.0001 all comparisons).

Conclusions

We conclude that both IgG1 and IgG2 are major determinants of IgG in patients with subnormal IgG1, combined subnormal IgG1/IgG3, or subnormal IgG3 and that in patients with subnormal IgG1 or combined subnormal IgG1/IgG3, median IgG2 levels are significantly lower in those with IgG < 7.00 g/L than those with IgG ≥ 7.00 g/L.

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Background

Immunoglobulin (Ig) G (IgG) is the predominant of five classes of Ig (IgG, IgA, IgM, IgE, and IgD). Igs differ in heavy chain structure and effector function [1]. IgG1, the largest IgG subclass, represents ~ 60% of IgG [1, 2] and has a half-life of 21 days [3]. Antibody responses to soluble protein and membrane antigens primarily induce IgG1 [1, 4], although polysaccharides and allergens also elicit IgG1 responses [1]. In two studies, adults with frequent or severe respiratory tract infection had subnormal IgG1 (< 2 standard deviations (SD) below respective means) in the absence of subnormal levels of other IgG subclasses, subnormal IgA, or subnormal IgM [5, 6].

In normal adults, IgG2 represents ~ 30% of serum IgG [1, 2]. IgG2 activates complement less readily than IgG1 and IgG3 [1], has low affinity for Fc receptors on phagocytes (FcγR) [1], crosses the placenta less freely than other IgG subclasses [7, 8], and has a half-life of 21 days [3]. IgG2 is the predominant antibody that responds to bacterial polysaccharide antigens [9,10,11,12]. Some persons with frequent or severe respiratory tract infection have subnormal IgG2 (< 2 SD below respective means) [13,14,15,16].

In normal adults, IgG3 represents ~ 4% of serum IgG [1, 17]. IgG3 activates complement more readily than other IgG subclasses [1], has high affinity for Fc receptors on phagocytes (FcγR) [1], crosses the placenta less readily than IgG1 and IgG4 but more so than IgG2 [18], and has an overall half-life of ~ 7 days [1, 3]. Some adults with frequent or severe respiratory tract infection have subnormal IgG3 (< 2 SD below respective means) [19,20,21].

IgG subclass deficiency (IgGSD) is characterized by frequent or severe upper or lower respiratory tract infection, one or more subnormal IgG subclass level(s) (≤ 2 SD below respective means) unexplained by other causes, and decreased IgG response to pneumococcal polysaccharide vaccination (PPSV) [20,21,22,23,24,25]. The predominance of women with IgGSD [21, 24, 25] becomes evident at ages ≥ 16 y [22]. IgGSD occurs in ~ 1 in 10,000 persons [26]. In two studies, IgG levels were subnormal in 38% and 46% of adults with IgGSD who had subnormal IgG1 only [5, 6] and in three adults with IgGSD and subnormal IgG2 in whom IgG1 levels were not subnormal [16]. These observations suggest that both IgG1 and IgG2 are determinants of IgG in adults with IgGSD.

We sought to identify factors associated with IgG levels in adults at diagnosis of IgGSD. We performed a retrospective chart and data review to identify adults diagnosed with IgGSD in a hematology clinic who had subnormal IgG1 only, combined subnormal IgG1/IgG3, or subnormal IgG3 only at diagnosis without other subnormal IgG subclasses, subnormal IgA, or subnormal IgM. We compiled these data: age at diagnosis; sex; autoimmune condition(s) (AC); atopy; serum levels of IgG, IgG subclasses, IgA, IgM; IgGsum (IgG1 + IgG2 + IgG3 + IgG4); and the D-parameter (D), the percentage difference between IgGsum and IgG [27]. In subnormal IgG1 only or combined subnormal IgG1/IgG3 subclass groups, we compared clinical and laboratory attributes of patients with and without IgG < 7.00 g/L. In each of the three subnormal Ig subclass groups, we analyzed relationships of IgGsum and IgG, performed backward stepwise regression on IgG and D using appropriate variables, computed correlations of IgG1 and IgG2, and determined IgG subclass proportions of IgGsum. We discuss the present results in the context of factors that influence IgG and IgG subclass levels in adults with IgGSD.

Results

39 adults with subnormal IgG1 only

General characteristics. There were 35 women (89.7%). IgG < 7.00 g/L was observed in 15 patients (38.5%). Clinical attributes of patients with IgG < 7.00 g/L and ≥ 7.00 g/L were similar, except that the prevalence of AC was significantly lower in patients with IgG < 7.00 g/L (Table 1). Mean IgG was significantly lower in patients with IgG < 7.00 g/L, by definition. Median IgG1 and median IgG2 were also significantly lower in patients with IgG < 7.00 g/L (Table 1).

Table 1 Characteristics of 39 adults with IgGSD and subnormal IgG1 onlya
Full size table

IgG and IgGsum

The difference between mean IgGsum and mean IgG was not significant (7.34 ± 1.31 g/L vs. 7.39 ± 1.27 g/L, respectively; p = 0.8816). The correlation of IgGsum and IgG was significant (Pearson correlation coefficient = 0.8063; adjusted r2 = 0.6406; p < 0.0001). Mean IgGsum was lower in patients with IgG < 7.00 g/L than IgG ≥ 7.00 g/L (6.40 ± 0.84 g/L vs. 7.93 ± 1.22 g/L, respectively; p < 0.0001). Mean D was also lower in patients with IgG < 7.00 g/L than IgG ≥ 7.00 g/L (− 11.0 ± 5.4 vs. 4.9 ± 8.7, respectively; p < 0.0001). Thus, the mean difference in IgG and IgGsum in adults with subnormal IgG1 only subgrouped by IgG1 levels (< 7.00 g/L vs. ≥ 7.00 g/L) was ~ 15.9%.

Regressions

Backward stepwise regression on IgG using age at diagnosis, sex, and IgG subclasses as independent variables revealed two positive associations: IgG1 (p < 0.0001) and IgG2 (p < 0.0001) (ANOVA p < 0.0001). This model accounted for 71.1% of the deviance of IgG. Backward stepwise regression on D using age at diagnosis and sex as independent variables revealed no significant associations.

53 adults with combined subnormal IgG1/IgG3

General characteristics. There were 47 women (88.7%). IgG < 7.00 g/L was observed in 32 patients (60.4%). Clinical attributes of patients with IgG < 7.00 g/L and ≥ 7.00 g/L were similar (Table 2). Mean IgG was significantly lower in patients with IgG < 7.00 g/L, by definition. Mean IgG1 and mean IgG2 were significantly lower in patients with IgG < 7.00 g/L (Table 2).

Table 2 Characteristics of 53 adults with IgGSD and combined subnormal IgG1/IgG3a
Full size table

IgG and IgGsum

Mean IgGsum and mean IgG did not differ significantly (6.94 ± 1.51 g/L vs. 7.12 ± 1.60 g/L, respectively; p = 0.5392). The correlation of IgG and IgGsum was significant (Pearson correlation coefficient = 0.9064; adjusted r2 = 0.8181; p < 0.0001). Mean IgGsum was lower in patients with IgG < 7.00 g/L than IgG ≥ 7.00 g/L (6.04 ± 0.73 g/L vs. 8.61 ± 1.35 g/L, respectively (p < 0.0001). Median D in patients with IgG < 7.00 g/L and those with IgG ≥ 7.00 g/L did not differ significantly (− 2.2 (− 32.3, 21.8) vs. − 2.7 (− 30.9, 9. 9), respectively; p = 0.1561).

Regressions

Backward stepwise regression on IgG using age at diagnosis, sex, and IgG subclasses as independent variables revealed two positive associations: IgG1 (p < 0.0001) and IgG2 (p < 0.0001) (ANOVA p < 0.0001). This model accounted for 82.5% of the deviance of IgG. Backward stepwise regression on D using age at diagnosis and sex as independent variables revealed no significant association.

115 patients with IgGSD and subnormal IgG3 only

General characteristics. Mean age of these patients was 47 ± 13 y. There were 105 women (90.3%). Clinical and laboratory attributes are displayed in Table 3.

Table 3 Characteristics of 115 adults with IgGSD and subnormal IgG3 onlya
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IgG and IgGsum

The difference between mean IgGsum and mean IgG was not significant (9.71 ± 2.01 g/dL vs. 10.00 ± 1.87 g/L, respectively; p = 0.2680). The correlation of IgGsum and IgG was significant (Pearson correlation coefficient = 0.8859; adjusted r2 = 0.7828; p < 0.0001).

Regressions

Backward stepwise regression on IgG using age at diagnosis, sex, and IgG subclasses as independent variables revealed two positive associations: IgG1 (p < 0.0001) and IgG2 (p < 0.0001) (ANOVA p < 0.0001). This model accounted for 80.7% of the deviance of IgG. Backward stepwise regression on D using age at diagnosis and sex as independent variables revealed no significant association.

IgG subclasses as percentages of IgGsum

IgG1 percentages of IgGsum were significantly lower and IgG2 percentages of IgGsum were significantly higher in patients with subnormal IgG1 subclass levels than in patients with subnormal IgG3 only (Table 4). Other comparisons of these data are displayed in Table 4, along with presentation of IgG subclass percentages of IgGsum in ostensibly healthy adults in four studies from the literature (Table 4). We also compared ratios of levels of IgG1, IgG2, and IgG3 subclasses to that of IgG4 for each subject group. This revealed that the ratio of IgG2: IgG4 is higher for the three present subject groups than has been reported in previous studies of ostensibly healthy adults (Table 4).

Table 4 IgG subclasses as percentages of IgGsuma
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Correlations of IgG1 and IgG2

In patients with subnormal IgG1 only, the Pearson correlation coefficient of IgG1 vs. IgG2 was 0.0277 (adjusted r2 =  ~ 0; p = 0.8816) (Fig. 1). In patients with combined subnormal IgG1/IgG3, the Pearson correlation coefficient of IgG1 vs. IgG2 was 0.2456 (adjusted r2 = 0.0419; p = 0.0762) (Fig. 2). In patients with subnormal IgG3 only, the Pearson correlation coefficient of IgG1 vs. IgG2 was 0.2185 (adjusted r2 = 0.0393; p = 0.0190) (Fig. 3).

Fig. 1
figure 1

Correlation of IgG1 and IgG2 in 39 adult patients with IgGSD and subnormal IgG1 only. Pearson correlation coefficient 0.0277 (adjusted r2 =  ~ 0; p = 0.8816)

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Fig. 2
figure 2

Correlation of IgG1 and IgG2 in patients with 53 adult patients with IgGSD and combined subnormal IgG1/IgG3. Pearson correlation coefficient 0.2456 (adjusted r2 = 0.0419; p = 0.0762)

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Fig. 3
figure 3

Correlation of IgG1 and IgG2 in 115 adults patients with IgGSD and subnormal IgG3 only. Pearson correlation coefficient 0.2185 (adjusted r2 = 0.0393; p = 0.0190)

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Elevated IgA in IgGSD patients

Elevated IgA levels (> 4.00 g/L, > 2 SD above the mean) were observed only in women (Tables 1, 2 and 3). Altogether, nine women (4.8%) and none of 20 men had elevated IgA (p = 0.6047).

Elevated IgM in IgGSD patients

Elevated IgM levels (> 2.30 g/L, > 2 SD above the mean) were observed only in women (Tables 1, 2 and 3). Altogether, 28 of 187 women (15.0%) and none of 20 men had elevated IgM (p < 0.0001).

Discussion

This study of adults with IgGSD demonstrates that both IgG1 and IgG2 are major determinants of IgG in patients with subnormal IgG1, combined subnormal IgG1/IgG3, or subnormal IgG3, after adjustment for other variables. In patients with subnormal IgG1 or combined subnormal IgG1/IgG3, we also demonstrate that median IgG2 levels are significantly lower in those with IgG < 7.00 g/L than those with IgG ≥ 7.00 g/L. In the present study, IgG < 7.00 g/L occurred in 39% of patients with subnormal IgG1 only and 60% of patients with combined subnormal IgG1/IgG3. These latter observations are consistent with two respective reports that IgG was subnormal (< 7.00 g/L) in 38% and 46% of adults with IgGSD who had subnormal IgG1 only without other subnormal IgG subclasses, subnormal IgA, or subnormal IgM [5, 6], contradicting previous suggestions that patients with low IgG1 will most likely be identified without IgG subclass testing [31, 32].

In the present patients with subnormal IgG1 subclass patterns, mean IgG1 was significantly lower in those with IgG < 7.00 g/L than IgG ≥ 7.00 g/L. Regressions on IgG revealed significant positive associations of IgG1, both in patients with subnormal IgG1 only and patients with combined subnormal IgG1/IgG3, after adjustment for other variables. In 12 adult patients with IgGSD and subnormal IgG2 and subnormal IgG, nine also had subnormal IgG1 [16]. These observations demonstrate that IgG1 is a major component of IgG in adults with IgGSD as it is in subjects unselected for subnormal IgG subclass levels [2, 4, 28,29,30].

IgG2 levels in the present patients were within reference limits, by definition. Regardless, mean or median IgG2 levels in patients with subnormal IgG1 subclass levels were significantly lower in patients with IgG < 7.00 g/L than in patients with IgG ≥ 7.00 g/L. Regressions on IgG revealed significant positive associations of IgG2 in both subnormal IgG1 subclass groups, after adjustment for other variables. In 12 adults with IgGSD selected for subnormal IgG2 levels who also had subnormal IgG, three had normal IgG1 [16]. These observations demonstrate that IgG2 is also a major component of IgG in adults with IgGSD as it is in normal subjects [1, 2, 4, 28,29,30]. In contrast, none of 115 adults with IgGSD and subnormal IgG3 only had subnormal IgG [20].

In patients with subnormal IgG1, the prevalence of AC was significantly greater in those with IgG ≥ 7.00 g/L than IgG < 7.00 g/L. This suggests that preferential synthesis of IgG1, IgG2, or both may occur as a consequence of one or more AC. In another study, respective mean serum levels of IgG1 were significantly higher and mean serum levels of IgG2 were significantly lower in patients with primary Sjögren syndrome (pSS), systemic lupus erythematosus (SLE), and systemic sclerosis than in healthy controls [33]. Two other studies found that serum IgG1, IgG2, and IgG3 levels were significantly higher in patients with pSS [34] and SLE [35] than in normal control subjects.

IgG1 percentages of IgGsum were significantly lower and IgG2 percentages of IgGsum were significantly higher in patients with subnormal IgG1 subclass levels than in patients with subnormal IgG3 only. Correlations of IgG1 and IgG2 values in patients with subnormal IgG1 subclass levels were not significant. Although the correlation of IgG1 and IgG2 was significant in patients with subnormal IgG3 only, the strength of the Pearson correlation coefficient was low. Taken together, these observations suggest that a) IgG1 and IgG2 subclass proportions of IgGsum and absence of significant correlation of IgG1 and IgG2 in the present patients with subnormal IgG1 subclass levels are consequences of the subnormal IgG1 selection criteria we used; and/or that b) that synthesis of IgG1 and IgG2 in adults with IgGSD and subnormal IgG1 subclass levels is not regulated in tandem.

IgG1, IgG2 and IgG3 molecules have polymorphic antigens known as Gm (gamma marker) allotypes on the constant regions of their respective γ1, γ2, and γ3 heavy chains encoded in IGHG loci (chromosome 14q32.33) [36, 37]. Some Gm allotypes are associated with different serum Ig levels. For example, the “normal” IgG2 range for persons with allotype G2m(23)- is 35% lower than that of persons with G2m(23) + [38]. There was a three-fold difference across mean serum IgG3 levels of normal adults grouped by G3m allotypes [29]. Few persons have deletions or other structural changes in IGHG loci that decrease the level of one or more IgG subclasses [39,40,41,42,43]. Most patients with IgGSD have dysfunctional regulation of IgG subclass production [44]. Intravascular distributions, fractional catabolic rates, and average biologic half-lives of IgG1 and IgG2 are similar [3].

All patients in this study presented with frequent or recurrent upper or lower respiratory tract infection and some of them were discovered to have subnormal IgG1 subclass levels. Adults in two other studies also had frequent or recurrent upper or lower respiratory tract infection and subnormal IgG1 only [5, 6]. In a California cohort of 78 adults with IgGSD, 27 (35%) had subnormal IgG1 (< 3.42 g/L), alone or in combination with subnormal IgG3 or IgG4 [21]. In a study of 3005 persons ≥ one year of age who had frequent or severe episodes of infection (and their relatives) and other patients without infection discovered incidentally to have hypogammaglobulinemia, 119 (4%) had subnormal IgG1 only [45]. Of these 119 patients, 83% had infections, especially sinusitis [45]. These and related observations [46] suggest that the proportion of adults with subnormal IgG1 who have or eventually develop frequent or severe respiratory tract infection is high.

Mean IgG2 was significantly lower in patients with IgG < 7.00 g/L than IgG ≥ 7.00 g/L in this study, although the IgG2 level of each patient was within the reference limit. Subnormal IgG2 is associated with frequent or severe respiratory infection in some persons [13,14,15,16], whereas other persons with subnormal or absent IgG2 are healthy [30, 40, 41, 47, 48]. Thus, it is unknown whether quantitative differences in IgG2 levels in the present patients contributed to their frequent or severe respiratory tract infection.

IgG3 exerts multiple effector functions against many viral and bacterial pathogens [1, 49]. Subnormal IgG3 only is the most common IgGSD pattern in adults [19,20,21, 25]. Nonetheless, IgG3 levels < 2 SD between population means are common in ostensibly healthy adults [2, 28,29,30] and in some patient groups unselected for frequent or severe respiratory tract infection or subnormal Ig [50,51,52].

The mean difference in IgG and IgGsum in the present adults with subnormal IgG1 only subgrouped by IgG1 levels (< 7.00 g/L vs. IgG ≥ 7.00 g/L) was ~ 16%. In another study, IgG and IgGsum differed by > 15% in 11% of 571 consecutive clinical samples [53]. The difference between IgG and IgGsum correlated with the proportion but not level of IgG1 [53]. After dilution of samples with differences > 15%, repeat testing did not reduce the differences significantly [53]. In the present study, we did not observe significant mean differences in D in adults with combined subnormal IgG1/IgG3 subgrouped by IgG1 levels (< 7.00 g/L vs. IgG ≥ 7.00 g/L).

Infection susceptibility was increased in persons with common AC [54,55,56,57,58] and atopy [59,60,61,62] who were unselected for IgGSD. The odds of respiratory tract infection were significantly increased in male Finnish military recruits with mannose-binding lectin levels below the median, after adjustment for asthma status [63]. In contrast, the prevalence of mannose-binding lectin ≤ 50 µg/L in white adults with IgGSD did not differ significantly from that in general European white populations [64]. In persons with subnormal IgE, the prevalence of frequent or severe respiratory tract infection [65, 66], other subnormal Ig isotypes [65, 67], and autoimmune conditions [66, 67] was significantly greater than that of control subjects. Hypogammaglobulinemia E in adults with IgGSD was negatively associated with bronchitis, allergic asthma, IgG1, and levels of blood CD4 + lymphocytes, after adjustment for other variables [68].

In this study, there was a predominance of women in all IgGSD groups, consistent with other reports of IgGSD in adults [6, 16, 19,20,21, 24, 45, 69]. The predominance of females among persons with IgGSD becomes evident at puberty [70]. AC are common in adults with IgGSD [6, 16, 19,20,21, 45] and women predominate among adults with AC [71, 72]. The prevalence of chronic rhinosinusitis in women, the most common respiratory tract infection in adults with IgGSD [21, 64], is twice that of men [73]. Taken together, it is plausible that factors related to the X-chromosome, X-chromosome inactivation, or hormonal differences between women and men could explain the predominance of women in cohorts of adults with IgGSD, although this is unproven.

Elevated IgA occurred in 5% of 187 women and no men in this study, although the difference in prevalence was not significant. Elevated IgA occurs in some patients with AC [74, 75] and others with cirrhosis due to chronic hepatitis B [76]. In healthy women and men grouped by age, there was no significant difference in mean IgA levels [77].

Elevated IgM occurred in 15% of 187 women and none of 20 men in this study. Elevated IgM levels are common in AC [78]. In 404 adults in the U.S. ages 20–89 y without conditions known to affect Ig levels, women had significantly higher IgM levels than men, regardless of age [77]. In a population-based survey of 460 adults in Spain, there was a significant negative association of male sex with IgM levels, after adjustment for other variables [79]. Serum IgM levels in adults are directly related to the number of X-chromosomes [80].

The present regression analyses demonstrate that IgG1 and IgG2 levels account for 71–82% of the variance of IgG levels in 207 adults with IgGSD. Thus, we infer that other factors not included in our analyses also influence IgG levels. We cannot exclude the possibility that AC, atopy, IgA, or IgM levels also influence IgG, although that possibility is not suggested by the results of the present univariate analyses. IgG subclass data from individual age- and sex-matched control subjects unselected for frequent or severe upper or lower respiratory tract infection or IgGSD were not available for analysis. Results in other IgGSD cohorts could vary due to referral differences and between-laboratory variation in methods of analysis, control data, and consequent IgG and IgG subclass reference limits. Ascertaining Gm allotypes, studying specific antibody activity, quantifying IgGSD responses to PPSV, and measuring IgE and mannose-binding lectin levels were beyond the scope of this work.

Conclusions

We conclude that both IgG1 and IgG2 are major determinants of IgG in patients with subnormal IgG1, combined subnormal IgG1/IgG3, or subnormal IgG3 and that in patients with subnormal IgG1 or combined subnormal IgG1/IgG3, median IgG2 levels are significantly lower in those with IgG < 7.00 g/L than those with IgG ≥ 7.00 g/L.

Methods

IgGSD definition

IgGSD was defined as frequent or severe respiratory tract infection, one or more subnormal IgG subclass level(s) (< 2 SD below respective means) unexplained by other causes, and decreased IgG response to PPSV [20,21,22,23,24,25]. Frequent respiratory tract infection was defined as four or more episodes per year that required antibiotic therapy. Severe respiratory tract infection was defined as any respiratory tract infection that required in-hospital treatment [81]. All patients were evaluated and diagnosed to have IgGSD during the interval November 1991–December 2019 using the same criteria [16, 20].

Patient selection

We reviewed the medical records of consecutive, unrelated, self-identified non-Hispanic white adults (ages ≥ 18 y) referred to a single outpatient hematology clinic (Southern Hematology & Oncology, P.C., Birmingham, AL, USA) because they had frequent or severe upper or lower respiratory tract infection inadequately managed with antibiotic and ancillary therapy, were subsequently diagnosed to have IgGSD, and had no first-degree relatives with IgGSD or other Ig deficiency previously known to this clinic as described in detail previously [16, 20, 25, 82]. Referring physicians diagnosed AC and atopy (allergic asthma, allergic rhinitis, allergic dermatitis/eczema). There are no Hispanic adults with IgGSD in our clinic population.

Patient exclusions

We excluded patients who reported therapy with daily oral corticosteroids [16]. We also excluded patients: who reported taking hydroxychloroquine [83,84,85,86]; captopril, carbamazepine, chloroquine, diphenylhydantoin, fenclofenac, gold, hydantoin, levamisole, penicillamine, sulfasalazine, valproic acid, or zonisamide [85]; oxcarbazapine [87]; leflunomide; methotrexate; or rituximab; with subnormal IgG2 [16] or subnormal IgA, or subnormal IgM; with monoclonal gammopathy; and with subnormal IgG subclass, subnormal IgA, or subnormal IgM levels due to other defined causes [16]. We also excluded patients with subnormal IgG4 because: (1) we desired to avoid introducing an additional IgG subclass variable; (2) substantial minorities of healthy men and women do not have detectable IgG4 [2, 88]; and (3) IgG4 levels measured by our laboratory that are > 2 SD below the lower reference limit are reported as zero.

Laboratory methods

IgG at diagnosis in each patient was measured using turbidimetry (Laboratory Corporation of America, Burlington, NC, USA). IgG subclasses were measured using four separate quantifications on corresponding specimens using rate nephelometry (Laboratory Corporation of America, Burlington, NC, USA) and reported separately from IgG. IgG and IgG subclasses were measured before IgG replacement therapy was initiated. For all Ig measurements, we defined mean ± 2 SD as reference limits [6, 89, 90]: IgG 7.00–16.00 g/L; IgG1 4.22–12.92 g/L; IgG2 1.17–7.47 g/L; IgG3 0.41–1.29 g/L; IgG4 0.01–2.91 g/L (0–2.9 g/L); IgA 0.70–4.00 g/L; and IgM 0.40–2.30 g/L. Ig reference ranges for diagnosis of IgGSD did not change during the interval 1991–2021. Subnormal Ig levels were defined as those below the corresponding lower reference limits. Subnormal Ig levels were documented twice in all adults at times they did not have acute infection. We used the second IgG subclass values for the present analyses.

Statistical analysis

Data for analyses consisted of observations on 207 adults: 39 with subnormal IgG1 only; 53 with combined subnormal IgG1/IgG3; and 115 with subnormal IgG3 only (see Additional file 1: Supplemental File "Observations in 207 Adults with IgGSD"). We evaluated continuous data for normality using d'Agostino's and Shapiro–Wilk tests. Descriptive data are displayed as enumerations, percentages, means (± 1 SD), or medians (range). Age and serum Ig data are expressed to the nearest integer. To determine factors that affect the percentage difference between IgGsum and IgG, we computed the D-parameter [27], defined as:

$$ D = \frac{IgGsum - IgG}{{IgGsum}} \cdot 100\% , $$

where IgGsum is the sum of IgG subclasses (IgG1 + IgG2 + IgG3 + IgG4) and IgG is total serum IgG.

Mean values of data from normal distributions were compared using Student's t test (two-tailed). Differences in median values of data from non-normal distributions were compared using the Mann–Whitney U test. We compared differences in proportions of dichotomous variables using Fisher's exact test (two-tailed). We compared some continuous data using Pearson’s correlation coefficient. We ranked the strength of statistically significant positive Pearson correlation coefficients as low (0.1–0.3), medium (> 0.3–0.5), and large (> 0.5–1.0).

The number of observations in each of the present IgGSD patient groups was relatively small and thus we minimized the numbers of independent variables we used in regression analyses [91]. For regressions on IgG, we included IgG subclass values and also age and sex because some IgG subclass levels in healthy adults are significantly influenced by these latter variables [88, 92]. For regressions on D, we used only age and sex as independent variables.

We defined values of p < 0.05 to be significant. Analyses were performed with Excel 2000® (Microsoft Corp., Redmond, WA, USA) and GB-Stat® (v. 10.0, 2003, Dynamic Microsystems, Inc., Silver Spring, MD, USA).

Availability of data and materials

All data generated or analysed during this study are included in this published article [and its Additional file 1].

Abbreviations

AC:

Autoimmune condition(s)

D:

D-parameter

IgGsum:

Sum of IgG subclasses

Ig:

Immunoglobulin

IgG:

Immunoglobulin G

IgGSD:

IgG subclass deficiency

PPSV:

Pneumococcal polysaccharide vaccination

SD:

Standard deviation

SLE:

Systemic lupus erythematosus

pSS:

Primary Sjögren syndrome

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Acknowledgements

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Funding

This study was supported in part by Southern Iron Disorders Center. The funding body played no role in the design of the study, the collection, analysis, and interpretation of data, or in writing the manuscript.

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Authors and Affiliations

  1. University of Alabama at Birmingham, Birmingham, AL, USA

    James C. Barton

  2. Southern Iron Disorders Center, Birmingham, AL, USA

    James C. Barton, Jackson Clayborn Barton, Luigi F. Bertoli & Ronald T. Acton

  3. Department of Medicine, Brookwood Medical Center, Birmingham, AL, USA

    James C. Barton & Luigi F. Bertoli

  4. Department of Microbiology, University of Alabama At Birmingham, Birmingham, AL, USA

    Ronald T. Acton

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Contributions

JaCB and LFB designed the study and evaluated and diagnosed all patients with IgGSD. JaCB, RTA, and JClB compiled and evaluated data and performed statistical analyses. All authors drafted, read, and approved the final manuscript.

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Correspondence to James C. Barton.

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Ethics approval and consent to participate

This work was performed according to the principles of the Declaration of Helsinki [93]. Western Institutional Review Board provided an exemption under 45 CFR 46.101(b)(4) pertinent to this study on 18 October 2018 (submission 2535878-44170911; 2 October 2018). Western Institutional Review Board waived a requirement to obtain informed consent because this study involved retrospective chart review and analyses of observations recorded in routine medical care and does not include personal identifier information.

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Supplementary Information

Additional file 1

. Observations in 207 Adults with IgGSD.

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Barton, J.C., Barton, J.C., Bertoli, L.F. et al. Factors associated with IgG levels in adults with IgG subclass deficiency. BMC Immunol 22, 53 (2021). https://doi.org/10.1186/s12865-021-00447-3

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BMC Immunology

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