Clinical and laboratorial profile and histological features on minor salivary glands from patients under investigation for Sjögren s syndrome

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Labial minor salivary gland biosy in Sjögren s syndrome Journal section: Oral Medicine and Pathology Publication Tyes: Research doi:10.4317/medoral.19486 htt://dx.doi.org/doi:10.4317/medoral.19486 Clinical and laboratorial rofile and histological features on minor salivary glands from atients under investigation for Sjögren s syndrome Débora-Lima Pereira 1, Verônica-Silva Vilela 2, Teresa-Cristina-Ribeiro-Bartholomeu dos-santos 3, Fábio- Ramôa Pires 4 1 DDS, Trainée, Oral Pathology, School of Dentistry, State University of Rio de Janeiro, Rio de Janeiro, Brazil 2 MD, Rheumatology, Pedro Ernesto University Hosital, State University of Rio de Janeiro, Rio de Janeiro, Brazil 3 DDS, MSc, Assistant rofessor, Oral Pathology, School of Dentistry, State University of Rio de Janeiro, Rio de Janeiro, Brazil 4 DDS, PhD, Adjunct rofessor, Oral Pathology, School of Dentistry, State University of Rio de Janeiro, Rio de Janeiro, Brazil Corresondence: Oral Pathology, School of Dentistry State University of Rio de Janeiro Av. 28 de setembro, 157 Vila Isabel - CEP: 20551-030 Rio de Janeiro/RJ- Brazil ramoafo@yahoo.com Received: 11/08/2013 Acceted: 19/10/2013 Pereira DL, Vilela VS, dos-santos TCRB, Pires FR. Clinical and laboratorial rofile and histological features on minor salivary glands from atients under investigation for Sjögren s syndrome. Med Oral Patol Oral Cir Bucal. 2014 May 1;19 (3):e237-41. htt://www.medicinaoral.com/medoralfree01/v19i3/medoralv19i3237.df Article Number: 19486 htt://www.medicinaoral.com/ Medicina Oral S. L. C.I.F. B 96689336 - ISSN 1698-4447 - eissn: 1698-6946 email: medicina@medicinaoral.com Indexed in: Science Citation Index Exanded Journal Citation Reorts Index Medicus, MEDLINE, PubMed Scous, Embase and Emcare Indice Médico Esañol Abstract Diagnosis of Sjögren s syndrome (SS) is comlex and the usefulness of labial minor salivary glands biosy in this rocess remains controversial. Objectives: to evaluate the clinical and laboratorial rofile and histological features on labial minor salivary glands from atients under investigation of SS. Study Design: clinical charts from 38 atients under susicion of SS and submitted to labial minor salivary glands biosies were reviewed. Clinical and laboratorial data were retrieved from the clinical files and the HE-stained histological slides were reviewed under light microscoy. Results: mean age of the atients was 56.5 years and 97% were females; histological analysis showed that 42% of the cases showed ductal dilatation, lymhocytic foci were found in 52.6% and, from this grou, 80% of the cases resented a foci/lobules ratio above 0.8. Acinar/ductal ratio was considered diminished in 39.5% of the samles. Thirty six (95%) and 32 (84%) atients, resectively, comlained about xerostomia and xerohthalmia. A study of the time interval of the symtoms that led to SS investigation showed a mean of 116 months. Moreover, sixty-six ercent of the atients had already been submitted to immunosuressive theray rior to the labial minor salivary gland biosy. Age of the atients, scintigrahic alterations on salivary function, antinuclear factor (ANF), anti-ro and anti-la did not show statistical significant association with the histological features. Lobules/foci ratio above 0.8 was the only histological arameter statistically associated with Sjögren s syndrome diagnosis (<0.0001). Conclusions: in the studied samle, lymhocytic foci on salivary glands were the only histological arameter associated to the diagnosis of SS. Early indication of labial minor salivary gland biosy to atients under investigation of SS could limit the effects of immunosuressive theray on the histological features associated with the evolution of salivary gland involvement in SS. Key words: Sjögren syndrome, minor salivary glands, biosy, lymhocytic foci. e237

Labial minor salivary gland biosy in Sjögren s syndrome Introduction Sjögren s syndrome (SS) is a chronic autoimmune disease characterized by xerohthalmia and xerostomia, functional alterations in both salivary and lacrimal glands and the resence of secific and unsecific serum autoantibodies in the affected atients (1-4). Diagnosis of SS is comlex and deends on subjective symtoms and clinical, serological and histological features, obtained through investigations erformed by a multidiscilinary team, including rheumatologists, ohthalmologists, clinicians and dentists (5-7). Biosy of labial minor salivary glands has been considered a diagnostic adjunctive technique with high secificity for SS, with few ost surgical comlications (8-10). Nevertheless, its regular use on SS diagnosis is not a routine at some reference centers, esecially due to the need for careful histological evaluation of the secimens and the invasive nature of the rocedure. The aim of the resent study was to retrosectively evaluate the clinical and laboratorial arameters and the detailed histological features of labial minor salivary glands from a grou of atients under investigation for SS. Material and Methods All secimens from biosies directed to the removal of labial minor salivary glands erformed in atients under investigation for Sjögren s syndrome registered in the Oral Pathology laboratory, School of Dentistry, State University of Rio de Janeiro, from 2006 to 2009 were reviewed. Histological slides containing hematoxylin and eosin (HE)-stained 5µm sections were analyzed under light microscoy (Eclise E-200 microscoe, Nikon, Jaan), according to the following criteria: number of salivary gland lobules; ercentage of adiose tissue on the salivary glands (less than 10% or more than 10%); absence or resence of ductal dilatation, acinar atrohy and sclerosis of the glandular connective tissue; acinar/ductal ratio (normal ratio, similar to normal glands; reduced ratio, with increased ductal comonent); the number of lymhocytic foci (1 focus was comosed of at least 50 groued lymhocytes); and the ratio number of lobules/number of foci. The established ratio as the limit between the grous considered comatible and non-comatible with the diagnosis of Sjögren s syndrome was 0.8, which means the resence of at least 5 lymhocytic foci in 4 minor salivary gland lobules. This criterion was used in addition to the absolute number of lymhocytic foci due to the fact that in some cases the submitted secimens were constituted by less than 5 salivary gland lobules. After selection and review of all HE-stained histological slides, clinical and laboratory information was retrieved from the clinical records of all atients on the Rheumatology service at Pedro Ernesto University Hosital, School of Medicine, State University of Rio de Janeiro. Data included age, gender, symtoms of xerostomia and xerohthalmia, results from the Schirmer tests and major salivary gland scintigrahy, history of recurrent arotitis, ulmonary involvement and resence of other concomitant rheumatoid autoimmune diseases. Serum laboratory data retrieved from the clinical records included autoantibodies, such as rheumatoid factor (RF), ANF, anti-ro and anti-la. Time interval with the symtoms that led to the investigation of Sjögren s syndrome and history of revious/resent immunosuressive treatment before the labial minor salivary gland biosies were also retrieved. Patients treated or under follow-u in other institutions, without clinical records resenting sufficient data for analysis, and showing HE-stained slides resenting no sufficient available tissue for histological analysis were excluded from the final studied samle. Data were tabulated and analyzed with the aid of the Statistical Package for Social Science (SPSS version 8.0, SPSS Inc., Chicago, Illinois, United States, 1997) with statistical significance level of 5% (<0.05). This study was aroved by the Ethics Committee, State University of Rio de Janeiro (COEP 059/2010). Results Seventy-seven HE-stained histological slides containing labial minor salivary glands from atients under investigation of Sjögren s syndrome were reviewed. From this initial samle, 38 cases resenting sufficient clinical and laboratory information were selected, reresenting the final studied samle. Patients from this grou resented a mean age of 56.5 years (ranging from 30 to 78 years) and 37 atients were females (97%). Histological analysis showed that 55.3% resented more than 10% of glandular adiose tissue and 42% of the cases showed ductal dilatation. Acinar atrohy and connective tissue sclerosis were found in 15.8% and 10.5% of the cases, resectively. Lymhocytic foci were found in 52.6% of the cases and, from this grou, 80% of the cases resented a foci/lobules ratio above 0.8. Acinar/ductal ratio was considered diminished in 39.5% of the samles. Figure 1 (A-D) shows some histological features from the affected minor salivary glands. Thirty six (95%) and 32 (84%) atients, resectively, comlained about xerostomia and xerohthalmia. Schirmer test was erformed in 29 atients (76%), of which 18 (62%) showed results comatible with Sjögren s syndrome. Eight out of the 38 atients (21%) reorted revious eisodes of recurrent arotitis and 20 out of the 33 atients (61%) submitted to salivary gland scintigrahy showed altered salivary function. Thirty two atients (84%) reorted being diagnosed with other autoimmune diseases, esecially rheumatoid arthritis, luus erythematosus and fibromyalgia, and 5 atients (13%) reorted associated ulmonary symtoms. Laboratory exams showed that out of the 32 atients tested e238

Labial minor salivary gland biosy in Sjögren s syndrome for ANF, 17 (53%) showed ositive results. In contrast, from the 24 atients who had been tested for RF, only 4 (17%) showed ositive results. Anti-Ro and anti-la were requested together for 24 atients and 9 (38%) showed ositive results for both. Time interval with the symtoms that led to Sjögren s syndrome investigation ranged from 1 to 288 months, with a mean of 116 months, and 25 out of the 38 atients (66%) had already been submitted to immunosuressive theray rior to labial minor salivary gland biosy. Time interval from the beginning of the symtoms and the labial minor salivary gland biosy ranged from 4 to 312 months, with a mean of 91 months. Table 1 shows the distribution of the histological arameters according to age, results from the salivary Fig. 1. A-B) Minor salivary glands showing extensive lymhocytic infiltration, destruction of the acinar comonent and reservation of the ductal structures (HE, 10x); C) Focal lymhocytic infiltration characteristic of Sjögren s syndrome (HE, 10x); D) Detail of the limit between the lymhocytic infiltrate and the reserved minor salivary gland acini (HE, 40x). Table 1. Distribution of the histological features observed on labial minor salivary glands according to clinical and laboratorial arameters. Ductal dilatation % Adiose tissue Acinar atrohy Acinar/ductal ratio Lobules/foci ratio Parameter Yes No <10% >10% Yes No NL * DE * <0,8 >0,8 Age (years) < 55 12 5 0.197 11 6 0.342 14 3 0.778 12 5 0.326 9 8 0.743 (n=38) > 55 10 11 10 11 18 3 11 10 13 8 Scintigrahy + 13 7 0.169 13 7 0.472 18 2 0.182 13 7 0.472 9 11 0.284 (n=33) - 5 8 6 7 9 4 6 7 9 4 ANF ** + 11 6 0.287 11 6 0.720 12 5 0.178 10 7 0.946 8 9 0.305 (n=32) - 6 9 8 7 14 1 9 6 10 5 RF *** + 3 1 0.590 1 3 0.272 2 2 0.179 0 4 0.020 0 4 0.093 (n=24) - 9 11 13 7 17 3 14 6 12 8 Anti-Ro + 5 3 0.673 4 4 0.685 7 1 0.955 4 4 0.182 4 4 0.657 (n=23) - 8 7 9 6 13 2 12 3 10 5 Anti-La + 4 1 0.339 2 3 0.618 4 1 0.539 3 2 0.621 2 3 0.343 (n=23) - 9 9 11 7 16 2 13 5 12 6 Diagnosis SS Yes 8 7 0.258 10 5 0.254 1 14 0.213 9 6 0.957 1 14 0.000 **** (n=38) No 8 15 11 12 5 18 14 9 21 2 * NL - normal, DE - decreased; ** ANF - antinuclear factor; *** RF - rheumatoid factor; **** SS - Sjögren s syndrome. e239

Labial minor salivary gland biosy in Sjögren s syndrome gland scintigrahy and laboratory arameters from the studied atients. Age of the atients, scintigrahic alterations on salivary function, ANF, anti-ro and anti- La did not show statistical significant association with the histological features. Although only 4 (17%) out of the 24 atients tested for RF resented ositive results, all showed reduced acinar/ductal ration and lobules/foci ratio over 0.8 (Table 1). It was also observed that 12 out of the 25 atients (48%) under use of immunosuressant rior to labial biosy showed a lobules/foci ratio over 0.8 and reduced acinar/ductal ratio. One third of the atients with negative results to anti-ro and anti-la showed a lobules/foci ratio over 0.8, but the resence of anti-ro and anti-la did not show statistical significant association with the resence of lymhocytic foci (=0.657 and 0.343, resectively). Lobules/foci ratio above 0.8 was the only histological arameter statistically associated with Sjögren s syndrome diagnosis (<0.0001). Out of the 38 atients, 16 (42%) showed lobules/foci ratio above 0.8, out of which 14 were diagnosed with Sjögren s syndrome after analysis of other criteria. One atient resented a lobules/ foci ratio lower than 0.8, but it was diagnosed with the syndrome due to the resence of other clinical and laboratorial arameters. Two atients were not diagnosed with Sjögren s syndrome, desite resenting a lobules/ foci ratio above 0.8, due to lack of confirmation after analysis of the other arameters (Table 1). Discussion SS is a comlex disease and diagnosis can be challenging in many cases. Deending on the country/region of origin of the study, SS can affect u 0.3 to 0.6% of the general oulation, with redilection for adult females on their 5th to 6th decades of life (2,3). It can be diagnosed as an isolated disease (rimary SS) or associated to other autoimmune diseases, such as rheumatoid arthritis and luus erythematosus (associated SS) (11,12). SS etiology remains unknown, but combined genetic and environmental factors seem to articiate in its athogenesis (2). Several clinical, laboratorial, imaginological and histological arameters have roved to be useful in SS diagnosis, and two different classification/diagnosis systems are currently being used for the disease, the American-Euroean Consensus Grou (13) and the Sjögren s International Collaborative Clinical Alliance (14). Both have considered labial minor salivary gland biosy as a useful tool for SS diagnosis, due to the ossibility of confirming the glandular damage and disease activity directly on the affected tissue. The resent study focused on evaluating the association of clinical and laboratorial arameters with histological features in a subset of atients under investigation of SS. As exected, the rofile of the samle was comosed of adult females, reinforcing the ossibility that hormonal and genetic alterations can, at least artially, modulate the develoment of the disease (7). Daniels et al. have recently reinforced the imortance of labial minor salivary gland biosy for SS diagnosis, due to its high secificity, allowing the analysis of disease activity directly on the target organ (9). Although some authors have considered labial minor salivary gland biosy an invasive rocedure, intraoerative roblems and ost-surgical sequelae are unusual (15). The most imortant limitation of the technique is the difficulty in establishing definite and objective histological diagnostic criteria caable of adequately characterize the secimens associated with SS. The athologist s individual subjective analysis can reveal considerable variability, even knowing that the resence of lymhocytic foci is considered the gold standard for SS diagnosis (9,16,17). Critical analysis of the detailed histological arameters is essential for the evaluation of their usefulness in SS diagnosis (18). The resent study focused on the evaluation of some histological arameters observed in minor salivary glands derived from labial biosies for SS diagnosis, but lymhocytic foci remained as the only statistically significant histological feature. It was interesting to notice that all atients resenting ositive RF showed a reduced acinar/ductal ratio and lobules/foci ratio above 0.8, but the low number of cases recludes any significance of these results. Analysis of a larger samle focusing on this arameter could offer new insights on this toic. Another limitation of the affected salivary glands analysis is associated with the large time interval from the beginning of the symtoms and the biosy. In the resent study the time interval from the first symtoms and the biosy showed a mean of 91 months, reinforcing this roblem. Patients usually start immunosuressive theray aimed at the control of the main symtoms and comlaints associated with the disease (esecially in associated SS) during this time interval, and it is believed that some histological arameters could be altered by local and systemic effect of the drugs. Zandbelt et al., have reorted alterations on the histological arameters in SS-affected minor salivary glands before and after corticosteroid theray, additionally suggesting that labial minor salivary gland biosy can be useful in monitoring activity of the disease (19). The results of the resent study showed that most atients had been submitted to or were on immunosuressive theray when the biosies were erformed. Even so, almost half the atients resented reduced acinar/ductal ratio and lobules/foci ratio above 0.8, fulfilling the histological criteria of SS. It is ossible to seculate that these values would have been higher if it were not for the interference of the immunosuressive theray. The imortance of serological autoantibodies, such as anti-ro and anti-la, on SS diagnosis has been demonstrated and, in the clinical ractice, serological exams e240

Labial minor salivary gland biosy in Sjögren s syndrome usually recede labial minor salivary gland biosy on routine SS diagnosis (13,15,20). The results of the resent study showed that more than 50% of the cases tested for anti-ro and anti-la resented negative results. However, about one third of such cases resented histological lymhocytic foci comatible with SS. This data reveals that without minor salivary gland biosy, a high ercentage of atients would remain underdiagnosed due to the lack of immunological criteria. These results are similar to the results from Langerman et al., which showed that only 53% of the atients who resented serological ositive results showed lymhocytic foci comatible with SS (18). The most reresentative histological feature associated with SS is the resence of lymhocytic foci. Bookman et al., have recently demonstrated the correlation of glandular fibrosis and reduction on salivary flow in SS affected atients (21). In the samles analyzed in the resent study, minor salivary gland connective tissue sclerosis as well as acinar atrohy, were found in solely 15.8% and 10.5% of the cases, resectively, restricting their correlation with the other arameters. It is imortant to oint out that these histological characteristics carry a variable subjective comonent during evaluation, limiting their routine use as an auxiliary arameter on SS diagnosis and rogression. A large recent multicentric study including clinical and histological data from 1726 subjects have demonstrated a strong association between the resence of lymhocytic foci on the affected minor salivary glands and serological arameters (higher titers of ANF, RF, anti- Ro and anti-la) and a weak correlation with subjective arameters, such as xerostomia and xerohthalmia (9). The results from the resent study showed no association of the clinical, serological and histological studied arameters. However, the limited number of cases and the long time interval for the indication of the labial minor salivary gland biosy in some cases under SS investigation may have modulated the results. In the studied samle, lymhocytic foci on salivary glands were the only histological arameter associated to the diagnosis of SS. Early indication of labial minor salivary gland biosy to atients under investigation of SS could limit the effects of immunosuressive theray on the histological features associated with the evolution of salivary gland involvement in SS. References 1. Rehman H. Sjögren s Syndrome. Yonsei Med J. 2003;44:947-54. 2. Delaleu N, Jonsson MV, Ael S, Jonsson R. New concets in the athogenesis of Sjögren s Syndrome. Rheum Dis Clin N Am. 2008;34:833-45. 3. Daniels TE. Sjögren s syndrome: clinical sectrum and current diagnostic controversies. Adv Dent Res. 1996;10:3-8. 4. Margaix-Muñoz M, Bagán JV, Poveda R, Jiménez Y, Sarrión G. Sjögren s syndrome of the oral cavity. Review and udate. Med Oral Patol Oral Cir Bucal. 2009;14:e325-30. 5. Scardina GA, Sanò G, Carini F, Sicola M, Valenza V, Messina P, et al. Diagnostic evaluation of serial sections of labial salivary gland biosies in Sjögren s syndrome. Med Oral Patol Oral Cir Bucal 2007;12:e565-8. 6. Lin DF, Yan SM, Zhao Y, Zhang W, Li MT, Zeng XF, et al. Clinical and rognostic characteristics of 573 cases of rimary Sjögren s syndrome. Chin Med J (Engl). 2010;123:3252-7. 7. Shiboski SC, Shiboski CH, Criswell L, Baer A, Challacombe S, Lanfranchi H, et al. American College of Rheumatology classification criteria for Sjögren s syndrome: a data-driven, exert consensus aroach in the Sjögren s International Collaborative Clinical Alliance cohort. Arthritis Care Res (Hoboken). 2012;64:475-87. 8. Caorali R, Bonacci E, Eis O, Bobbio-Pallavicini F, Morbini P, Montecucco C. Safety and usefulness of minor salivary gland biosy: retrosective analysis of 502 rocedures erformed at a single center. 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Acknowledgements The authors wish to thank FAPERJ and CNPq for financial suort for this study. e241