The clinical hallmarks of this disease are recurrent, necrotic, and indolent infections of soft tissues, primarily involving skin, mucous membranes, and the intestinal tract. Superficial infections of body surfaces may invade locally or systemically. Typical small, erythematous, nonpustular skin lesions often progress to large, well-demarcated, ulcerative craters (or pyoderma gangrenosa), which heal slowly or with dysplastic eschars. Staphylococcal or gram-negative enteric bacterial organisms may be cultured from such lesions for several weeks, despite antimicrobial therapy. Septicemia progressing from omphalitis associated with delayed umbilical cord severance has been observed in several families. Perirectal abscess or cellulitis leading to peritonitis or septicemia has been reported in multiple patients, and facial or deep neck cellulitis has been observed to progress from ulcerative mucous membrane lesions of the oral cavity. Recurrent invasive candidal esophagitis, erosive gastritis, acute appendicitis, and necrotizing enterocolitis have been reported in multiple patients. Recurrent otitis media occurs commonly, and progression to mastoiditis and facial nerve paralysis has been reported. Other common respiratory infections include severe bacterial (pseudomonal) laryngotracheitis, recurrent pneumonitis, and sinusitis. Severe gingivitis or periodontitis is a major feature among all patients who survive infancy. Acute gingivitis has appeared in all cases upon the eruption of the primary dentition. Subsequently, these patients develop characteristic features of progressive generalized prepubescent periodontitis, including gingival proliferation, defective recession, mobility, pathologic migration, and advanced alveolar bone loss associated with periodontal pocket formation and the partial or total loss of both the deciduous and permanent dentition.

The recurrent infections observed in affected patients appear to reflect a profound impairment of leukocyte mobilization into extravascular inflammatory sites. Skin windows and biopsy samples of infected tissues demonstrate inflammatory infiltrates totally devoid of neutrophils. The histopathologic feature is particularly striking, because marked peripheral blood leukocytosis (9 to 20 times normal values) is a constant feature of this disorder. Transfusions of leukocytes result in the appearance of donor neutrophils and monocytes in skin windows and skin chambers. The dysregulated healing of traumatic or surgical wounds observed in several patients represents a clinical feature not generally observed in patients with neutropenia or dysfunctional neutrophils. Unusual, paper-thin or dysplastic cutaneous scars have been found in some patients and, in one patient with a unique CD18 mutation, hypertrophic scars occurred.

The severity of infectious complications among LAD patients appears to be related directly to the degree of glycoprotein deficiency. Severely affected patients have essentially undetectable expression of all three alpha–beta (αβ) complexes in their neutrophils. Moderately deficient patients express 2% to 25% of all three αβ complexes. Patients with severe deficiency have either died in infancy or have demonstrated a susceptibility to severe, life-threatening systemic infections (peritonitis, septicemia, pneumonitis, aseptic meningitis). In contrast, among the patients expressing some functional CD11/CD18 integrins, life-threatening infections have been observed infrequently despite a relatively prolonged survival (greater than 50 years). In some moderately affected patients, skin lesions may disappear after the first few years of life, recurring only with occasional infections. Severe gingivitis always is observed in these patients and may be the presenting symptom. Delayed umbilical cord separation occurs more frequently in patients with the severe phenotype, but it is not universally found.

Suggested therapeutic guidelines for LAD are based on limited clinical experience. Although infectious complications generally are observed on body surfaces, life-threatening systemic infections may occur at any time, especially in individuals who fail to express any CD18 integrins. Superficial inflammatory lesions must be managed aggressively, with local care and antibiotic therapy. This is of special importance, because inflammatory signs may be minimal before the development of septicemic episodes. Moreover, the impaired healing of superficial
wounds appears to allow indolent colonization and subsequent reinfection. Early use of empiric combination therapy with a staphylocidal agent and an aminoglycoside is justified in acutely ill or febrile patients, in the absence of localizing findings. The use of prophylactic antibiotics may be advised. Limited clinical experience suggests that the number of systemic infections in patients with LAD is considerably diminished through the use of prophylactic regimens. Leukocyte transfusions have been used successfully in several patients with LAD; enhancement of inflammatory functions and clinical resolution of even life-threatening infections have been achieved in a clinical setting in which systemic antibiotic or surgical interventions were ineffective.

Bone marrow transplantation (BMT) with successful engraftment and apparent clinical recovery from disease has been achieved in several patients. Because of the inherent risks and expense, this approach should be considered only for patients with the severe phenotype of disease. Among patients undergoing transplantation, recipients of HLA-identical as well as HLA-mismatched (e.g., haplotype match) bone marrow have shown successful engraftment. In some cases, mixed but stable chimerism between donor and recipient cells is apparent 3 to 5 years after transplantation. In these cases, normal or slightly diminished blood granulocyte function is observed in vitro, and the patients demonstrate no clinical complications.

The identification in LAD patients having CD18 mutations raises the possibility that the introduction of a normal CD18 gene into hematopoietic cells could cure this disease, especially in light of the encouraging results of BMT. Some reports document the successful transfection or retroviral-mediated infection of LAD cells or cell lines with a normal CD18 cDNA, resulting in normal CD18 protein expression and normal cell adherence properties. Thus, the stage is set for future attempts at somatic cell gene therapy in LAD.

Neutrophils from each patient studied have demonstrated morphologic abnormalities, including a severe or total deficiency of specific granules and a variety of nuclear abnormalities, such as bilobed or multilobed nuclei or nuclear blebs, clefts, or pockets. Diminished or absent neutrophil lactoferrin content has been confirmed in only three cases, and the membrane marker alkaline phosphatase has been shown to be diminished or absent in the neutrophils of all but one reported case. Total cellular content and release of the secondary granule markers (lactoferrin, B12 transport protein, cytochrome b, and lysozyme) have been shown to be diminished when assessed in selected patients, although the levels of primary granule constituents (myeloperoxidase, beta-glucuronidase) generally are normal. Among recognized cases, somewhat heterogeneous abnormalities in cellular functions have been observed. Chemotaxis and intracellular microbial activity represent the most consistently reported functional deficits.

The deficiency of specific granules is suggested by a history of recurrent cutaneous, subcutaneous, mucous membrane, or pulmonary infections caused by S. aureus, virulent gram-negative enteric bacteria, or species of Candida. Findings of abnormal morphology and abnormally weak cytochemical reactions for alkaline phosphatase are highly suggestive of this disorder. Cytochemical and ultrastructural studies to confirm the diminished numbers or abnormal morphology of specific granules and their specific constituents establishes a diagnosis.

Sequence analysis of DNA from a patient with secondary granule deficiency revealed a five base-pair deletion in the second exon of the transcription factor CCAAT/enhancer binding protein–ε (C/EBPε) locus. A second patient had a one base-pair insertion, and the predicted frame shifts resulted in truncations of the 32-kD major C/EBPε isoform, with loss of the dimerization domain, DNA binding region, and transcriptional activity. The phenotypic and functional defects of neutrophils from C/EBPε-deficient mice closely parallel those of the human syndrome of specific granule deficiency. The multiple functional defects observed in early neutrophil progenitor cells are apparently the consequence of C/EBPε deficiency. Specific granule deficiency is thus a defect in myelopoiesis, because C/EBPe is required for the promyelocyte–myelocyte transition in myeloid differentiation.