Infectious Complications of Antibody Deficiency

Primary antibody deficiencies are the most common inherited immunodeficiencies. Secondary antibody deficiencies are also increasingly common complications of some chronic diseases and pharmacotherapy. Antibody deficiency disorders are characterized by reduced or absent serum immunoglobulins, recurrent and severe infections caused by certain bacteria and viruses, and, in some cases, autoimmunity and an increased predisposition to cancer.

Immunoglobulin (Ig) molecules consist of two identical light chains and two identical heavy chains held together by disulfide bonds. There are two types of light chains (κ and λ) and five classes, or isotypes, of heavy chains (IgG, IgA, IgM, IgD, and IgE), as well as 4 subclasses of IgG (IgG1-4) and 2 subclasses of IgA (IgA1 and IgA2). The antigen-binding amino-terminal variable regions of the Ig molecule are unique for each B lymphocyte clone. The carboxyl-terminal constant region is the same for each isotype or subclass.

Antibodies bind to specific antigens through the variable region of the Ig molecule. The constant region performs effector functions such as activation of complement, binding to a phagocytic cell, or antibody-dependent cell-mediated cytotoxicity. In some circumstances, the antigen-specific binding region functions alone by blocking the binding of a toxin or an infectious agent to the surface of a target cell. Different antibody isotypes are more or less efficient at providing effector functions.

B lymphocytes develop from a pluripotent precursor stem cell to an IgM-expressing immature cell in the bone marrow, a process that does not require contact with antigen ( Fig. 102.1 ). Further differentiation to mature B lymphocytes and to memory B-cells or plasma cells takes place in peripheral lymphoid organs beginning about 1 week after antigen stimulation. Activated B lymphocytes can undergo a change in isotype expression from IgM to IgG, IgA, or IgE. Genes encoding variable regions can also undergo somatic hypermutation, a process that increases the affinity of antigen binding by antibody. Re-exposure to an antigen results in an accelerated memory (or secondary) immunologic response; this is responsible for the more rapid and greater magnitude of Ig responses to “booster” vaccinations compared with primary antigen exposures.

Primary humoral immunodeficiencies have a prevalence of 13.9–18.1 per 100,000 persons in the US. The classification of these disorders was updated in 2019 by the International Union of Immunological Societies ( Table 102.1 ), and diagnostic criteria for some have been established. Mutations can reduce the expression of receptors and signaling molecules essential for B-cell development, prevent class-switch recombination to different isotypes and subclasses, or impair the survival or function of B cells. Many of these disorders display considerable clinical variability, even among persons with the same mutation. These phenotypic differences may be the result of environmental or epigenetic modulation of gene expression.

TABLE 102.1

Primary Immunodeficiencies Predominantly Involving Antibody Deficiency

Immunologic Characteristics	B lymphocyte Numbers	Serum Immunoglobulins	Known Genetic Defects and Inheritance	Clinical Features
Very low or absent B lymphocytes Serum immunoglobulins low or absent(Agammaglobulinemia syndromes)	<1% of normal	All isotypes low or absentNo specific antibody responses	X-linked - BTK	Severe and recurrent bacterial and enteroviral infections, chronic diarrhea
			AR— IGHM, CD179A, CD179B, BLNK, IGLL1, PIK3CD, PID3R1, TCF3, SLC39A7, LRRC8A	Severe infections, cytopenias, autoimmunity, poor growth, rash
			AD— TCF3, TOP2B	Recurrent bacterial infections, congenital facial and limb anomalies
Normal or low B lymphocyte numbers >1 Serum Ig isotype reduced(Common variable immunodeficiency syndromes)	Normal or low	IgG decreased, IgA usually decreased, IgM variable No or poor antibody response	Many unknown X-linked —ATP6AP1, SHEKBP1, KM2TD	Severe bacterial infections, cirrhosis, low serum copper, cognitive impairment, cytopenias, congenital anomalies, developmental delay
			AD— PIK3CD gain of function, PIK3R1, PTEN , TNFRSF13B, ICOS, TNFRSF13C, TNFSF12, NFKB1, NFKB2, IKZF1, IRF2BP2, SEC61A1, CTLA4, KDM6A	Severe infections, recurrent sinopulmonary infections, cytopenias, lymphadenopathy, lymphoproliferation, autoimmunity, warts, lymphoma, leukemia, cognitive impairment, congenital anomalies
			AR— CD19, CD81, CD20, CD21, TNFRSF13B, TNFRSF13C, TRNT1, ARHGEF1, RAC2, MOGS, LRBA	Recurrent infections, autoimmunity, sideroblastic anemia, recurrent fever, eye abnormalities, deafness, neurocognitive disorders, congenital anomalies
Normal B lymphocyte numbers Low IgG and IgA Normal or elevated IgM(Hyper-IgM syndromes)	Normal	IgG and IgA decreased, IgM variable No or poor antibody response	AD— AICDA	Recurrent bacterial infections, lymphadenopathy
			AR— AICDA, UNG, INO80, MSH6	Recurrent bacterial infections, lymphadenopathy, autoimmunity, cancer predisposition
Normal B lymphocyte numbers (Selective Ig deficiencies)	Normal	Selective isotype and/or subclass deficiency— One or more isotypes/subclasses absent Usually normal antibody responses IgG subclass ± IgA deficiency may have poor antibody responses	Unknown AR—Ig heavy chain	Most asymptomatic. IgG subclass ± IgA and selective IgA deficiency may have recurrent bacterial infections Selective IgM deficiency may have recurrent bacterial infections
	Normal	Selective IgA deficiency— Low or absent IgA Other isotypes normal Normal antibody responses	Unknown	Most asymptomatic. Bacterial infections, autoimmunity
	Normal	κ Light chain deficiency— κ Light chains absentNormal antibody responses	AR— IGKC	Asymptomatic
	Normal	Selective antibody deficiency Ig concentrations normal Poor antibody responses	Unknown	Asymptomatic, or bacterial infections
	Normal	Transient hypogammaglobulinemia of infancy Low IgGNormal immune responses	Unknown	Asymptomatic, or recurrent infections, rarely severe infections, improvement over time

AD, autosomal dominant; AR, autosomal recessive.

Antibody-mediated or humoral immunity is particularly important in the defense against infection caused by polysaccharide-encapsulated bacteria such as Streptococcus pneumoniae and Haemophilus influenzae, as well as some viruses (poliovirus, non-polio enteroviruses, herpesviruses) and protozoa ( Giardia lamblia ) . In some antibody deficiency disorders, immunodeficiency is present prenatally, but transplacental transfer of maternal IgG in pregnancy protects infants against infection in the first several months of life. Children with severe antibody deficiency typically become symptomatic after passively transferred immunity wanes. The onset of other humoral immunodeficiencies can be delayed, and some may be progressive. Among children, the average prevalence of humoral immunodeficiencies is highest in those aged 1–5 years (29–67 per 100,000).

Approach to the Patient With A Suspected Antibody Deficiency

A primary antibody deficiency should be considered in children with recurrent or chronic sinopulmonary infections, particularly in association with (1) poor growth, (2) unusual or unusually severe infections, (3) chronic or recurrent diarrhea, (4) a family history of recurrent and severe infections or of early childhood deaths, or (5) granulomatous or autoimmune disease. Physical features suggesting humoral immunodeficiency include absent or small lymph nodes and tonsils, chronic lymphadenopathy, a dermatomyositis-like rash, or hypertrophic osteoarthropathy.

Timely diagnosis of primary antibody deficiency and institution of immunoglobulin replacement therapy reduces the morbidity and mortality associated with these disorders. Quantitative serum immunoglobulin concentrations should be compared with normal values for age and reduced levels of IgG, IgM, or IgA (or normal levels in the presence of a clinical picture strongly suggestive of antibody deficiency) should prompt additional investigations ( Fig. 102.2 ). ^, B lymphocytes (CD19 ⁺ ) and other lymphocyte subsets are quantified by flow cytometry and should be compared with normal values for age. The ability to generate a specific antibody response is assessed by measuring serum isohemagglutinins (naturally occurring antibodies to ABO blood group antigens) and antigen-specific serum antibody concentrations before and after vaccination with protein (e.g., tetanus, diphtheria, pertussis) and polysaccharide antigens (e.g., pneumococcal polysaccharide vaccine in children >2 years). Quantifying IgG subclasses may be helpful in some cases, but the wide range of normal values and an inconsistent correlation between low serum concentrations and clinical disease complicate the interpretation of results, particularly in younger children. B lymphocyte and immunoglobulin levels obtained during acute severe illness should be interpreted with caution and abnormal results confirmed after recovery. Evidence of the decreased expression or function of a specific gene product may be useful, but these tests generally are available on a research basis only. A definitive diagnosis is possible for disorders caused by known genetic mutations. Carrier detection and prenatal diagnosis is also possible in some cases.

FIGURE 102.2, Algorithm for the evaluation of common primary antibody deficiency disorders. Ab, antibody; PS, polysaccharide.

Patients with primary antibody deficiencies and severe symptoms should receive immunoglobulin replacement therapy, which reduces the rate and severity of infections. The half-life of IgG varies based on clinical status and is significantly shortened during severe illness. Ideally, trough serum IgG concentrations (immediately before the next administration of immunoglobulin) should be within the normal range of healthy persons. Increasing use has been made of rapid subcutaneous infusion and home or infusion center programs. Immunoglobulin replacement therapy does not prevent all infections, and signs and symptoms of infection should be evaluated promptly and breakthrough infections treated aggressively. Some patients, particularly those with frequent or chronic respiratory infections, may benefit from prophylactic antibacterial therapy. Patients with hyper-IgM syndrome (HIGM) caused by CD40L or CD40 deficiency have an increased susceptibility to Pneumocystis jirovecii infection and should receive trimethoprim-sulfamethoxazole or other effective prophylaxis. Vaccines composed of live-attenuated virus vaccines should not be administered to patients known or suspected of having a primary antibody deficiency.

Agammaglobulinemias: Severely Reduced IgG, IgA, and IgM With Absent B Lymphocytes

The prototype of antibody deficiency syndromes is X-linked agammaglobulinemia (XLA), which has an incidence of approximately 1 in 200,000 persons and accounts for about 85% of cases of agammaglobulinemia ( Box 102.1 ; Table 102.1 ,). ^, XLA is caused by mutations in the Bruton tyrosine kinase gene, Btk, which is required for the normal differentiation of pro-B cells to pre-B cells and mature B lymphocytes. ^, A family history of male relatives with recurrent infections is common, but about one half of patients represent new mutations. The severity of infectious complications can also differ among family members. Prenatal diagnosis and carrier detection are possible if the mutation is known. Rare autosomal recessive and autosomal dominant agammaglobulinemias result from mutations in other genes important to B cell development.

BOX 102.1

Agammaglobulinemia

Clinical Presentation

Onset in infancy or early childhood
Recurrent respiratory and invasive infections, especially Haemophilus influenzae type b, Streptococcus pneumoniae
Chronic diarrhea, malabsorption, chronic Giardia, and rotavirus infection
Chronic enteroviral meningoencephalitis, poliomyelitis, dermatomyositis-like syndrome
Neutropenia with infection
Lymph nodes and tonsils absent or small

Diagnosis

IgG, IgM, and IgA >2 standard deviations below mean for age
Peripheral blood CD19 ⁺ B lymphocytes <2%
Poor specific antibody responses, including isohemagglutinins
Genetic testing

Treatment

Immunoglobulin replacement

Serum IgG, IgA, and IgM levels are very low (>2 standard deviations [SD] below the mean value for age), and patients have poor or no specific antibody responses following infection or immunization. Circulating CD19 ⁺ B lymphocytes are absent or present in very low numbers (generally <2%). Plasma cells are absent from lymph nodes and bone marrow, and lymph nodes and tonsils are absent or small. T lymphocytes are normal in both number and function. Neutropenia can occur in association with acute infections.

Transplacentally acquired maternal IgG typically protects infants with agammaglobulinemia from infection in the first few months of life. Thereafter, affected children have recurrent bacterial infections, particularly otitis media, sinusitis, and pneumonia. More than one half of patients are symptomatic by 1 year of age and almost all by 5 years of age. Other invasive bacterial infections (septicemia, meningitis, osteoarticular infections) are also common. Encapsulated bacteria, particularly H. influenzae type b (Hib), S. pneumoniae, Staphylococcus aureus, and Pseudomonas spp. cause most infections. Up to 50% of patients experience chronic diarrhea, steatorrhea, or malabsorption, in some cases associated with chronic rotavirus and G. lamblia infections. ^, The incidence of enteritis due to Salmonella spp. and Campylobacter jejuni is higher in persons with agammaglobulinemia than the general population. Persistent Mycoplasma and Ureaplasma infections of the respiratory tract, joints, and urogenital tract also occur.

Although children with antibody deficiencies usually manifest greater susceptibility to bacterial than to viral infections, some children with agammaglobulinemia have severe and chronic enteroviral infections. In regions of the world where wild-type or live-vaccine-strain polioviruses circulate, paralytic disease in patients with agammaglobulinemia can occur. Meningitis caused by non-polio enteroviruses can have an insidious onset with ataxia, loss of cognitive skills, and paresthesias, or present more acutely with fever, headache, and seizures. Central nervous system (CNS) enterovirus infection can be the initial manifestation of XLA and can occur despite intravenous IgG (IGIV) replacement therapy. Cerebrospinal fluid (CSF) pleocytosis with a lymphocytic predominance, increased protein levels, and, frequently, decreased glucose levels is typical, although some children have normal or only mildly abnormal findings. CSF abnormalities tend to worsen with clinical exacerbations. Some individuals with chronic enteroviral infections develop a dermatomyositis-like syndrome characterized by muscle weakness, edema and woody induration of the skin, and a violaceous rash over the extensor surfaces of joints, often accompanied by hepatitis.

The prognosis of XLA has greatly improved with IGIV therapy, particularly when it is initiated at an early age. Aggressive and prolonged treatment of bacterial infections is critical. Patients with chronic enteroviral meningoencephalitis are treated with high doses of IgG (to maintain trough levels of >1000 mg/dL) or with plasma or immune serum known to have high antibody titers to the enterovirus causing the infection. Intrathecal IGIV has also been used. The most common causes of death among patients with agammaglobulinemia remain chronic enteroviral and pulmonary infections.

Common Variable Immunodeficiency Disorders: Severely Reduced IgG, IgA, and/or IgM With Normal or Low Numbers of B Lymphocytes

Common variable immunodeficiency disorder (CVID) represents a heterogeneous group of disorders characterized by low serum Ig concentrations, defective production of specific antibodies, and an increased susceptibility to respiratory and gastrointestinal tract infections ( Box 102.2 ). ^, ^, ^, ^, CVID affects 1 in 30,000 persons and has an equal prevalence in males and females. Persons with CVID have serum total IgG concentration ≥2 SD below the mean for their age, a marked decrease in IgM and/or IgA, and impaired specific antibody responses. ^, Numbers of peripheral B lymphocytes may be normal, reduced, or increased; the clinical phenotype exhibited by an individual patient generally correlates with the numbers and subtypes of peripheral B lymphocytes. Current diagnostic criteria restrict the definitive diagnosis of CVID to persons >4 years of age, in part owing to the need to exclude other immunodeficiencies that manifest early in life. CVID can develop in persons who initially have clinical and laboratory findings suggestive of selective IgA or IgG subclass deficiencies. Immunodeficiency can be progressive, and patients must be followed longitudinally; up to 10% of patients develop opportunistic infections. ^,

BOX 102.2

Common Variable Immunodeficiency

Clinical Presentation

Onset 2 years of age to adulthood
Recurrent and severe sinopulmonary infections, especially Streptococcus pneumoniae, Haemophilus influenzae
Gastrointestinal infections, especially Giardia, Campylobacter jejuni, Salmonella spp.
Chronic Mycoplasma infection
Severe infections due to hepatitis C, cytomegalovirus, varicella-zoster virus, enteroviruses
Autoimmune and inflammatory disorders (gastrointestinal lymphoid hyperplasia, inflammatory bowel disease, autoimmune cytopenias, arthritis, vasculitis)
Lymphoid hyperplasia, splenomegaly, peripheral lymphadenopathy
Increased risk for lymphoma, gastric carcinoma

Diagnosis

IgG usually >2 standard deviations below mean for age; young children may present with progressive IgG subclass deficiency
IgA usually >2 standard deviations below mean for age
IgM normal or low
Peripheral blood CD19 ⁺ B lymphocytes normal or reduced
Poor specific antibody responses, absent isohemagglutinins
Genetic testing available for some forms

Treatment

Immunoglobulin replacement

Approximately 25% of cases of CVID are familial. While many mutations have been described, almost all are uncommon, and the genetic basis of most CVID is not known. Most have autosomal recessive inheritance; some forms have distinctive associated features. Other immunodeficiencies, including agammaglobulinemia, class switch recombination defects, X-linked lymphoproliferative disease, and “leaky” severe combined immunodeficiency syndromes may resemble CVID. Certain drugs, chromosomal abnormalities, infection, malignancy, protein losing states, and systemic illnesses are associated with secondary CVID ( Table 102.2 ).

TABLE 102.2

Secondary Antibody Deficiency–Causes, Features and Clinical Impact

Category	Situation/agent	Features	Risk	Interventions
Physical losses	Pulmonary: chylothorax, exudative pleural effusion. GI: PLE, intestinal lymphangiectasia, IBD. Renal: nephrotic syndrome. Skin: severe atopic dermatitis, burns	Predominantly decreased IgG, sometimes decreased IgA and IgM. Poor vaccine responses	Moderately increased risk of bacterial infections. Rare opportunistic infections	Treat underlying condition. Rarely immunoglobulin replacement
Medical conditions	Malnutrition	Decreased secretory IgA. IgG generally preserved.	Moderately increased risk of bacterial infections Cryptosporidium Candida spp.	Treat underlying condition
	B-cell lymphoproliferative disorders: lymphoma, leukemia, myeloma, MDS, Waldenstrom macroglobulinemia	Decreased IgG, IgA and/or IgM. Poor vaccine responses	High risk of fungal, viral and opportunistic bacterial infections	Treat underlying condition. Antimicrobial prophylaxis. Rarely immunoglobulin replacement
	Solid organ transplant	Decreased IgG. Poor vaccine responses	High risk of fungal, viral and opportunistic bacterial infections	Antimicrobial prophylaxis. Rarely immunoglobulin replacement
Immunosuppressant drugs	Glucocorticoids	Decreased B- and T- cell numbers. Decreased IgG and/or IgA	High risk of fungal, viral and opportunistic bacterial infections	Decrease or discontinue agent if possible. Antimicrobial prophylaxis. Rarely immunoglobulin replacement
Immunosuppressant drugs	Calcineurin inhibitors: cyclosporine, tacrolimus. mTOR inhibitors: sirolimus. Antiproliferative agents: mycophenolate mofetil, azathioprine	Decreased B-cell numbers. Decreased IgG and/or IgA. Permanent IgA deficiency associated with cyclosporine. Poor vaccine responses	High risk of fungal, viral and opportunistic bacterial infections	Decrease or discontinue agent if possible. Antimicrobial prophylaxis. Rarely immunoglobulin replacement
	Antineoplastic: methotrexate, cyclophosphamide, mercaptopurine	Decreased B- and T-cell numbers. Decreased IgG and/or IgA	High risk of fungal, viral and opportunistic bacterial infections
	Small-molecule kinase inhibitors: ibrutinib, imatinib, dasatinib	Decreased IgG. Little effect on vaccine responses	Increased risk of bacterial, fungal and viral infections
	Anti-CD20: rituximab, ofatumumab Anti-CD22: inotuzumab Anti-CD19: blinatumomab Anti-CD19 chimeric antigen receptor antibodies	Variable effects. Decreased IgG. Poor vaccine responses	Increased risk of bacterial, fungal and viral infections, including M. tuberculosis , HBV, CMV, HSV reactivation Rare opportunistic infections
	Anti-thymocyte globulin	Decreased IgG, IgA and/or IgM. Poor vaccine responses	Moderately increased risk of bacterial infections	Immunoglobulin replacement. Antimicrobial prophylaxis
	Anti-inflammatory IL-1 inhibitors: anakinra, rilonacept	Decreased IgG. Decreased B- and T-cell numbers	High risk of fungal, viral and opportunistic bacterial infections	Antimicrobial prophylaxis. Rarely immunoglobulin replacement
	Anti-cytokine antibodies: tocilizumab (IL-6), siltuximab (IL-6)	Decreased IgG	Increased risk of bacterial, fungal and viral infections, including tuberculosis	Decrease or discontinue agent if possible. Rarely immunoglobulin replacement
Other drugs	Antiepileptic: phenytoin, carbamazepine, valproic acid, zonisamide, lamotrigine	Decreased IgA	Usually asymptomatic. May have increased bacterial and Giardia infections	Decrease or discontinue agent if possible. Rarely immunoglobulin replacement
	Anti-inflammatory: penicillamine, sulfasalazine, hydroxychloroquine, gold	Decreased IgA and sometimes IgG	Usually asymptomatic. May have increased bacterial and Giardia infections	Decrease or discontinue agent if possible. Rarely immunoglobulin replacement

CMV, cytomegalovirus; GI, gastrointestinal; HBV, hepatitis B virus; HSV, herpes simplex virus; IBD, inflammatory bowel disease; Ig, immunoglobulin; IL, interleukin; MDS, myelodysplastic syndrome; mTOR, mammalian target of rapamycin; PLE, protein-losing enteropathy.

Symptoms of CVID are unusual in children under 2 years of age. Bimodal peaks of incidence are recognized at 2–5 and 16–28 years of age. Patients most commonly have recurrent sinopulmonary infection, chiefly due to bacteria such as S. pneumoniae, H. influenzae, Moraxella catarrhalis, and M. pneumoniae. Recurrent pneumonia sometimes progresses to bronchiectasis. Invasive bacterial infections occur in 10%–25%. Enteric infections caused by Giardia, C. jejuni, and Salmonella spp. are frequent and can be more severe and prolonged than in immunocompetent persons. Chronic genitourinary tract, joint, and systemic infections caused by Mycoplasma spp. have been described. Although most viral infections are not complicated in patients with CVID, increased frequency and severity of hepatitis C virus, cytomegalovirus (CMV), measles, and varicella-zoster virus infection have been reported. ^, Complications of enteroviral infection, including chronic encephalomyelitis and dermatomyositis-like syndrome, occur but are less frequent than with the agammaglobulinemias.

Allergic disorders are found in over 30% of children and adolescents with CVID. Inflammatory or autoimmune diseases occur in 20%–35% of patients and can cause more serious morbidity than infections. Diffuse and pulmonary granulomatous disease, lymphocytic interstitial pneumonitis, and chronic lymphadenopathy are reported in 10%–20% of patients. Inflammatory bowel disease, lymphonodular hyperplasia, or nonspecific malabsorption affect up to 25% of patients; immune cytopenias and hematological disorders, such as autoimmune thrombocytopenia, hemolytic anemia, neutropenia, and pernicious anemia occur in 10%. About one fourth of patients have significantly reduced growth. The incidence of some cancers, particularly lymphomas and gastric carcinoma, is markedly elevated in patients with CVID, but onset is predominantly in adults.

Most patients with CVID require IG replacement therapy. Prophylactic antibiotics may benefit some patients, particularly those with recurrent respiratory infections and bronchiectasis. Patients require careful monitoring for autoimmune and lymphoproliferative complications.

Hyper-IgM Syndromes (Hims, Class Switch Recombination Defects): Reduced IgG and IgA With Normal or Elevated IgM and Normal Numbers of B Lymphocytes

Children with hyper-IgM syndromes (HIMS) have recurrent or serious infections in the first 5 years of life, absent or low levels of serum IgG, normal or elevated serum IgM, absent or poor specific immune responses, normal or elevated numbers of B lymphocytes, and normal numbers of T lymphocytes ( Box 102.3 ). ^, ^, ^, ^, HIMS is rare, affecting about 1 in 300,000 persons. Approximately 65% of cases are inherited in an X-linked recessive fashion and are due to mutations of the gene encoding CD40L ( TNFSF5 ). ^, ^, Rare mutations of CD40 ( TNFRSF5 ) cause a similar disorder with autosomal-recessive inheritance. Both CD40 and CD40L deficiency are associated with impaired humoral and cellular immunity. Mutations of AICDA are responsible for autosomal recessive and autosomal dominant forms of HIMS, and mutations in UNG , INO80, and MSH6 cause autosomal recessively inherited forms that are not associated with significant cellular immunodeficiency.

BOX 102.3

Class Switch Recombination Disorders (Hyper-IgM Syndromes)

Clinical Presentation

Onset in infancy or early childhood
Recurrent and severe sinopulmonary infections
Pneumocystis jirovecii infection
Severe or chronic Cryptosporidium and Giardia infections
Neutropenia, parvovirus-induced aplastic anemia
Autoimmune and lymphoproliferative disorders (sclerosing cholangitis, diabetes, arthritis, inflammatory bowel disease, uveitis)

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