Sialendoscopic management of autoimmune sialadenitis: a review of literature.

Autoimmune diseases of major salivary glands include Sjögren's syndrome and a complex of disorders classified as immunoglobulin G4-related diseases. These pathologies are characterised by an autoimmune reaction mediated by T-helper lymphocytes that targets the ducts of exocrine glands in Sjögren's syndrome and glandular parenchyma in immunoglobulin G4-related diseases. Immunoglobulin G4-related diseases represent recently introduced multi-organ diseases that also involve the salivary glands. However, the morbid conditions once known as Mikulicz's disease and Kuttner's tumour were recently considered as two variants of immunoglobulin G4-related diseases affecting the major salivary glands ( immunoglobulin G4-related sialadenitis). This review briefly summarises the pathogenesis and clinical features of autoimmune diseases of the major salivary glands, focusing on the diagnostic and therapeutic role of sialendoscopy. © Copyright by Società Italiana di Otorinolaringologia e Chirurgia Cervico-Facciale, Rome, Italy.

Introduction

Salivary gland diseases include neoplasms and non-neoplastic disorders such as viral parotitis, sialolithiasis and chronic non-lithiasic sialadenitis. Autoimmune diseases are responsible for a small share of chronic, non-lithiasic inflammatory disorders of major salivary glands. In these conditions, the parenchyma of salivary glands, salivary ducts, or both represent the target of an attack carried out by the immune system against its own tissues, through autoantibodies and T cells. Sjögren's syndrome (SS) and immunoglobulin G4-related diseases (IgG4-RD) are the main chronic autoimmune sialadenitis .

SS attacks the exocrine glands, specifically the salivary and lacrimal tissue, and CD4+ lymphocytes play the main role in the autoimmune process. IgG4-RD are newly described fibro-inflammatory conditions that often present as nodular lesions that can affect nearly every organ system . In IgG4- RD, the target of the autoimmune attack is the connective tissue and the inflammatory cell infiltration is composed of IgG4-positive plasma cells, CD4+ and CD8+ T cells. In recent years, both Mikulicz's disease (MD) and the so-called Kuttner's tumour (KT) were classified in the group of IgG4- RD and considered as variations of IgG4 RD affecting salivary tissue (IgG4-related sialadenitis or IgG4-RS) .

The aim of this review is summarise the characteristics of the autoimmune diseases that affect the salivary glands, analysing the potential role of sialendoscopic techniques in the diagnosis and treatment of these conditions.

SjÖgren's syndrome (SS)

SS may be defined as a chronic autoimmune inflammatory exocrinopathy affecting the salivary and lacrimal glands. The dysfunction of exocrine glands is usually accompanied by a multitude of extraglandular manifestations . SS may occur as primary or secondary form. Primary SS, with or without extraglandular involvement, occurs in the absence of another underlying rheumatic disorder, whereas secondary SS is associated with another autoimmune disease, such as systemic lupus erythematosus, rheumatoid arthritis, or scleroderma. Given the overlap of SS with many other rheumatic disorders, it is sometimes difficult to determine whether a clinical manifestation is solely a consequence of SS or is due to one of its overlapping disorders. These primary and secondary types occur with similar frequency, but sicca complex symptoms seem to be more severe in primary form , .

Primary SS is an autoimmune disorder characterised by lymphocytic infiltrates with destruction of exocrine glands and systemic production of autoantibodies against ribonucleoprotein particles SS-A/Ro and SS-B/La. The infiltrating cells (T- and B-cells, dendritic cells) interfere with salivary production at several points, starting a vicious circle and causing the salivary glands to become sites of chronic inflammation .

Despite extensive studies, the underlying cause of SS and its pathogenesis remains controversial. It is thought that environmental factors can trigger inflammation in individuals with a genetic predisposition, configuring a multifactorial disease .

Primary SS is strongly associated with HLA-DR3 and the linked genes B8, and DQ2, and C4A null gene. Within the primary SS group, those with anti-La represent a subset that show an even more striking association with HLA 3. This suggests that the anti-La-positive patients with SS may be the most homogeneous subgroup, both clinically and immunogenetically. Anti-Ro is associated with DR2 and the linked DQ1 gene, as well as with DR3, and this may reflect the wider diagnostic associations of this antibody. Rheumatoid arthritis with secondary SS is associated with DR4 rather than DR3 -.

Viruses are viable candidates as environmental triggers, although no single virus has been implicated and the triggering mechanisms is still unknown. Epstein-Barr virus, HTLV-1, human herpesvirus 6, HIV, hepatitis C virus and cytomegalovirus may have a role and clinical manifestations of sicca syndrome are frequently seen in patients infected with HIV, HTLV-1, and hepatitis C -. Damage and/or cell death due to viral infection may provide triggering antigens to toll-like receptors in or on dendritic or epithelial cells, which, by recognising pathogen-associated patterns, are activated and begin producing cytokines, chemokines and adhesion molecules. As T and B lymphocytes migrate into the gland, they themselves become activated by dendritic and epithelial cells, thereafter acting as antigen-presenting cells. Expressed antigens include SSA/ Ro, SSB/La, alpha-fodrin and beta-fodrin, and cholinergic muscarinic receptors. Dendritic cell triggering by immune complexes formed from SSA–anti-SSA (or other immune complexes) may propagate the ongoing innate and acquired immune activation -.

SS is one of the most common autoimmune rheumatic diseases with a prevalence around 1% according to the revised American-European Consensus Group (AECG) criteria . There is general agreement that it is a disease of middle-aged or elderly women (mean age of onset 45–55 years, male/female ratio 1:9) .

Clinically, most individuals with SS present with sicca symptoms (xerophthalmia and xerostomia), that are expression of chronic exocrinopathy. The lack of saliva in the mouth and the absence of a normal 'pool' of saliva underneath the tongue causes an increase in the rate of caries and may promote oral candidosis. In more severe cases, the tongue is atrophic, fissured or even ulcerated. Parotid glands are frequently swollen. Exocrine glands other than the salivary and lacrimal glands may be affected. Dry skin and dry hair are symptoms frequently elicited on direct questioning. About 30% of patients have diminished vaginal secretions and may present with dyspareunia. Involvement of the gastrointestinal tract leads to reflux oesophagitis or gastritis owing to a lack of protective mucus secretion is also possible - .

SS is a systemic disease. About 70% of patients complain of fatigue that may be misdiagnosed whereas arthritis, with characteristics similar to those seen in rheumatoid arthritis, occurs in about 30% of subjects . The renal features of SS include interstitial nephritis, leading to renal tubular acidosis, and membranous glomerulonephritis due to circulating immune complex disease (more common in the secondary SS). The incidence of significant renal disease of around 5%, but subclinical renal features of disease rises to around 30% . Interstitial pneumonitis determined by an interstitial infiltrate of lymphocytes around the bronchioles may cause function abnormalities found in approximately 25% of patients with SS . Although vasculopathies such as Raynaud's phenomenon and congenital heart block are also frequently observed, these disorders assume minor clinical significance . Conversely, neurological involvement is quite rare (1%), but may manifest as multiple sclerosis-like syndrome . Finally,it has long been known that patients with primary SS have a 44-fold increased risk of mucosa-associated lymphoid tissue (MALT) type B cell lymphoma .

A number of classification criteria for SS were designed, primarily for clinical research studies, but are also used to guide clinical diagnoses. The revised AECG criteria for classification of Sjögren's syndrome , summarised in Table I, were proposed in 2002 and are the most commonly used criteria for diagnosis of SS. A new set of classification criteria has been developed by the Sjögren's International Collaborative Clinical Alliance (SICCA) investigators and accepted as a provisional criteria set by the American College of Rheumatology (ACR) in 2012 .

Table I.

American–European Consensus Group Classification criteria for Sjögren's syndrome. Diagnosis of primary Sjögren's syndrome requires four of six criteria; in addition, either criterion number 5 or criterion number 6 must be included. Sjögren's syndrome can be diagnosed in patients who have no sicca symptoms if three of the four objective criteria are fulfilled. Secondary Sjögren's syndrome is diagnosed when, in the presence of a connective-tissue disease, symptoms of oral or ocular dryness exist in addition to criterion 3, 4, or 5.

1.	Ocular symptoms	Dry eyes for more than 3 months Foreign-body sensation Use of tear substitutes more than 3 times daily
2.	Oral symptoms	Feeling of dry mouth Recurrently swollen salivary glands Frequent use of liquids to aid swallowing
3.	Ocular signs	Schirmer test performed without anesthesia (< 5 mm in 5 min) Positive vital dye staining results
4.	Oral signs	Abnormal salivary scintigraphy findings Abnormal parotid sialography findings Abnormal sialometry findings (unstimulated salivary flow < 1.5 mL in 15 min)
5.	Positive minor salivary gland biopsy findings (focus score ≥1)
6.	Positive anti–SSA or anti–SSB antibody results
Exclusions: any patient with past head and neck radiation treatment, hepatitis C infection, acquired immunodeficiency disease (AIDS), pre-existing lymphoma, sarcoidosis, graft versus host disease, use of anticholinergic drugs.

Diagnostic workup in the suspicion of SS usually include the blood tests listed in the revised AECG criteria. Furthermore, patients with SS frequently present leucopenia, thrombocytopenia, high ESR and anti-nuclear antibodies. The classical histological feature of SS at minor salivary gland biopsy is of at least one 'focus' of 50 or more (predominantly CD4+) T lymphocytes per high-powered field clustered around a salivary duct (periductal focal lymphocytic infiltrates). Histology reports sometimes describe a generalised scattering of inflammatory cells across the gland usually described as a 'chronic sialadenitis'. The report may conclude that this is 'compatible with SS'. In fact, chronic sialadenitis can be found in normal individuals and this should be classed as a negative biopsy . AECG criteria order to objectively assess xerophthalmia through simple, economic tests such as Rose Bengal staining and the Schirmer test, which can be used to strongly support or refute the suspicion of SS . Conversely, the tests recommended to objectify the signs of xerostomia, except for the poor standardised sialometry, are particularly expensive (salivary scintigraphy) and not very specific (sialography) imaging techniques. Sialographic changes in parotid glands affected by SS were accurately described and, with regards to chronic sialadenitis, classified into punctate, globular, cavitary and destructive sialectasia of the acinar and ductal system. These four sialectasic changes are thought to represent increasing glandular damage caused by an autoimmune reaction .

Sialendoscopy, according to AECG criteria, is not listed as a recommended examination to assess salivary gland involvement in SS. The reason for this exclusion is probably due to historical reasons: the revised AECG criteria, in fact, date to 2002 whereas sialendoscopy still represents a relatively new procedure. However, this technique allows endoscopic transluminal visualisation of major salivary glands and offers a mechanism for diagnosing and treating both inflammatory and obstructive pathologies related to the ductal system, and thus like sialography potentially adequate to recognise the ductal abnormalities accompanying SS .

In the literature, there is little experience about the role of sialendoscopy in SS. Some authors report the presence of hyperaemia at the level of main and the second-order salivary ducts, with evidence of a vascular pattern demonstrating perivascular inflammation and congestion . It is possible that this endoscopic appearance, also observed in recurrent parotitis, could characterise the initial phases of SS, whereas the pale, little vascularised appearance of the ductal wall expresses the subsequent progression of the disease, in which parenchymal tissue is replaced by fibrosis . Obstructive mucous plugs are frequently observed in the ductal tree. The presence of these obstructions causes saliva stagnation and inflammation upstream of the obstruction, which is probably responsible for the occasional parotid swelling and pain . However, stricture formation was found to be the major cause of ductal obstruction by other authors. Jager, et al. and De Luca, et al. reported the presence of stricture in the majority of salivary glands affected by SS explored in their study . Microlithiasis, related to the subsequent inflammatory episodes , is observed mainly in the advanced stages of the disease in which the fibrous replaced and subverted the entire gland. Our research group is currently investigating a possible role of sialendoscopy in diagnosis of SS by analysing the expression of IL-17 and IL-23 in saliva and ductal lavage collected during the surgical procedure. The therapy for SS is based on drugs aimed to modulate the autoimmune response. Traditional immunomodulatory drugs such as low-dose steroids, methotrexate, ciclosporin and azathioprine show no benefit, while there is some evidence to support the use of hydroxychloroquine sulphate, although there is no evidence of a direct effect on salivary or lacrimal flow -. Thus, although biologic agents represent promising treatments -, the current management of xerostomia and xerophthalmia is still based on topical treatments (tear and saliva substitutes) and sialogogues such as pilocarpine and cevimeline -.

During sialendoscopy, a semi-rigid miniaturised endoscope is inserted into the salivary duct after dilating the papilla and driven in the ductal system under constant irrigation 40. Sterile saline solution is the fluid of choice for the irrigation of salivary ducts, but corticosteroid solutions can also be used - Thus, a diagnostic procedure alone causes relevant dilation of the entire ductal system. On the other hand, the use of interventional sialendoscope with working channels allows the concomitant treatment of strictures, mucus plugs and sialoliths, contributing to alleviate complaints in patients affected by inflammatory disease -. Recent clinical experience suggested that sialendoscopy may alleviate the oral symptoms of SS by restoring salivary function -. Jager, et al. conducted a randomised study of 20 patients with SS oral symptoms who were randomly assigned to the nonintervention control group or to the sialendoscopy group. In patients undergoing sialendoscopy, unstimulated and stimulated saliva flow, Clinical Oral Dryness Score, Xerostomia Inventory Score, and EULAR Sjogren's Syndrome Patient Reported Index score showed a significant improvement of symptoms at 1 and 8 weeks after the procedure . Although a positive effect of sialendoscopy on xerostomia cannot be assessed with a few, small case series, these promising results suggest that sialoendoscopy could be a viable technique to treat obstructive salivary gland diseases related to SS that is refractory to conventional management.

IgG4-related sialadenitis (IgG4-RS)

IgG4-RD are newly described fibro-inflammatory conditions that often presents as tumefactive lesions affecting several districts. Hamano, et al. first recognised IgG4-RD in 2001, after a connection between elevated serum IgG4 levels and inflammatory mass lesions in the pancreas causing autoimmune pancreatitis . However, an initial consensus statement regarding diagnosis of IgG4-RD was reached only in 2011 during the first international symposium for IgG4-RD .

The head and neck region is the second most common site for presentation of IgG4-RD after the pancreas and some pseudotumoural diseases of unknown pathogenesis, including MD and KT, have been attributed to IgG4-RD during the last 10 years -. Identification of IgG4-positive plasma cells in both KT and MD propelled renewed interest in these diseases, and fueled re-analyses of the classification of inflamed salivary glands .

The exact aetiology of IgG4-RS is unknown and no known role of the IgG4 molecule has been identified. IgG4 itself normally represents the smallest fraction of IgG subclasses (< 5%). It has an amino acid variance in the hinge region allowing it to split and randomly combine with other half molecules, creating asymmetric bispecific antibodies with two different antigen-binding sites. For this special feature, IgG4 scarcely forms immune complexes, binds Fc-receptors and complements component with low affinity. Thus, its ability to initiate immune responses is limited .

It is postulated that the inflammatory and fibrotic processes that drive IgG4-RS are propagated by a combination of T helper (Th) 2 cells and regulatory T cells (Treg cells). This is contrary to most autoimmune disorders where polarised Th1 and/or Th17 subsets are responsible for the inflammatory process .

Clinical data on IgG4-RS are increasingly reported. Currently, it is believed that this condition preferentially affects middle-aged males presenting with persistent parotid and/or submandibular gland swelling, unilaterally or bilaterally.

The disorder that was identified by Kuttner in 1896 commonly involves one or both submandibular glands, clinically presenting as hard tumour-like masses with tendency to nodular swelling that can be confounded with malignant forms. The disease is often associated with microlithiasis. Histological sections reveal preservation of the lobular architecture, marked lymphoplasmacytic inflammation, large irregular lymphoid follicles with expanded germinal centers and acinar atrophy without prominent lymphoepithelial lesions. Characteristically, prominent cellular interlobular fibrosis due to activated fibroblasts and infiltration of lymphocytes and IgG4-positive- stained plasma cells is observed. Eosinophil infiltration and obliterative phlebitis are frequent .

MD, first described in 1888 , refers to idiopathic, bilateral, painless, symmetrical and persistent swelling of the lacrimal, parotid and submandibular glands. Because MD and primary-SS are histologically similar, MD has long been considered as a subtype of SS. Upon haematoxylin-eosin staining, lacrimal or salivary gland specimens from MD showed severe mononuclear cell infiltration and lymphoid follicles around the ductal and acinar cells. The infiltration of numerous IgG4-positive plasmacytes near acinar and ductal cells and around lymphoid follicles allows differentiating MD from SS . Therefore, the presence of IgG4-positive plasmacytes in the inflammatory infiltration suggests that MD and KT are only two different phenotypes of IgG4-RS. A comparison between clinical and histological features of the two phenotypes of IgG4-RS and SS is summarised in Table II.

Table II.

Comparison between SS and IgG4-RS.

Features		SS	IgG4-RS
			MD phenotype		KT phenotype
Clinical	Gender (female:male) Glands involvement Bilateral/unilateral Appearance Salivary impairment Response to steroids	9:1 Both parotids and submaxillary glands Bilateral Usually transient swelling Severe Limited	Both parotids and submaxillary glands Bilateral Persistent symmetrical swelling	1:2.5 Mild Good	submaxillary glands Often unilateral Persistent nodular swelling
Histological	Fibrosis Obliterative phlebitis IgG4+ plasmacytes	Inconstant, mild Absent Absent		Constant, intense frequent >30–50 hpf
Serological	Serum IgG4 levels Serum IgE levels Anti-Ro(SSA)/ Anti-La(SSB)	Normal Normal High rate		High High Absent
Imaging	Ultrasound	Inhomogeneity hypoechoic areas and hyperechoic lines and spots	Inhomogeneity hypoechoic areas and hyperechoic lines and spots		Nodular, smooth contour mass with hypoechoic foci scattered against a heterogeneous background.

Clinically, xerostomia is inconstant in IgG4-RS, involving approximately 30% of patients. Autoimmune pancreatitis, sclerosing cholangitis and asthma are frequently associated conditions (15-30%). Lacrimal gland involvement, as well as sinonasal disorders and cervical lymphadenopathy (70%), are frequent coexisting conditions .

Imaging studies of salivary glands show a pattern of nonspecific features in MD phenotype of IgG4-RS. On US examination of the affected glands, hypoechoic areas with hyperechoic lines creating a reticular pattern that is a common finding in patients affected by SS. On the contrary, a nodular pattern with duct enlargement and microlithiasis is often observed in the disorder once known as KT. Computerised tomography and magnetic resonance imaging have lower diagnostic accuracy compared to ultrasonography -.

Biopsy of the affected gland is necessary to formulate a diagnosis of IgG4-RS, although lip biopsy has been proposed as an alternative technique . There are three main histopathological hallmarks for IgG4-RD: infiltrates of IgG4+ plasmacytes, intense fibrosis and obliterative phlebitis. However, the exact histological findings vary greatly depending on the tissue affected and clinical presentation. Currently, histologic diagnosis of IgG4-RD is based primarily on IgG4 positive to IgG containing cell ratio and, secondarily, on the number of IgG4 positive cells per high power field. A ratio of IgG4 to IgG that is higher than 50% and the confirmation of at least 30 IgG4-positive cells per high-power field are considered to be highly suggestive of IgG4-RD .

Laboratory tests on blood can confirm the diagnosis. Patients affected by IgG4-RD show significantly higher total IgG, IgG2, IgG4 and IgE. In addition, eosinophil counts are usually increased and hypocomplementaemia is frequent. In particular, elevated serum IgG4, even if neither present in all patients with histologically proven IgG4-RD nor specific for it, can be a supplementary tool in the diagnosis of IgG4-RD . Serum IgG4 concentration > 135 mg/dl-1 have been defined as a threshold value for diagnosis . Furthermore, it was observed that IgG4 serum concentration correlates with reduction of saliva production and glandular fibrosis, suggesting that IgG4 concentration in serum can represent a useful marker to follow the evolution of the disease and efficacy of treatment .

In the literature, there are very few publications focusing on medical treatment of IgG4-RS, although all authors indicate systemic steroid therapy as first-line treatment and prednisone represents the most used drug. In the past decades, in fact, the good responsiveness to steroids was considered a distinctive clinical feature of MD compared to SS .

Steroid therapy, weighted according to the activity of the disease and body mass, is usually long-term and the initial dose is gradually tapered after 2-4 weeks of starting therapy. Long-term glucocorticoid treatment seems to significantly improve symptoms related to reduced salivary secretion conferring, according to some studies, recovery of histological abnormalities. Some authors have emphasised the role of early steroid therapy to improve outcomes in patients with IgG4-RS. Salivary secretion rate, indeed, seems to decrease with histological changes related to a delayed intervention . Conversely, the role of other immunosuppressive agents such as azathioprine, methotrexate, or mycophenolate mofetil is still controversial and understudied.

To the best of our knowledge, there are no reports about sialendoscopy performed in patients affected by IgG4 related sialadenitis. However, we believe that this technique will be useful in the management of patients suffering from IgG4-RD. Although it is unlikely that this method can replace the role of the biopsy for diagnostic purposes, sialendoscopy is a potential tool in the treatment of sialadenitis. Endoscopic techniques, in fact, as is the case in other chronic sialadenitis, could eliminate microlithiasis and debris thorough rinsing or using microforceps and basket, also allowing the treatment of eventual ductal stenosis using hydrostatic pressure or high-pressure balloons. Furthermore, the intraductal administration of antiinflammatory drugs, while poorly studied at present, may be an alternative to systemic steroids in the future.

Conclusions

The role of sialendoscopy in the treatment of autoimmune chronic sialadenitis is currently understudied, mainly due to the recent worldwide diffusion of this technique.

The outcomes of a few preliminary trials, however, are particularly encouraging and deserve to be verified in randomised controlled trials with a larger sample and longer follow-up period.

The discussion between otolaryngologists and rheumatologists should also be more incisive so that sialendoscopy and sialography can be considered as useful techniques for diagnosis and staging of autoimmune diseases of the salivary glands. Furthermore, rheumatologists should consider a minimally invasive technique such as interventional sialendoscopy for management of patients suffering from autoimmune diseases of the major salivary glands who do not derive benefit from conventional therapies.