Oral changes in individuals undergoing hematopoietic stem cell transplantation

Barrach, Regina Haddad; Souza, Mair Pedro de; Silva, Daniela Polo Camargo da; Lopez, Priscila Suman; Montovani, Jair Cortez

doi:10.1016/j.bjorl.2014.04.004

Abstracts

INTRODUCTION:

Patients undergoing hematopoietic stem cell transplantation receive high doses of chemotherapy and radiotherapy, which cause severe immunosuppression.

OBJECTIVE:

To report an oral disease management protocol before and after hematopoietic stem cell transplantation.

METHODS:

A prospective study was carried out with 65 patients aged > 18 years, with hematological diseases, who were allocated into two groups: A (allogeneic transplant, 34 patients); B (autologous transplant, 31 patients). A total of three dental status assessments were performed: in the pre-transplantation period (moment 1), one week after stem cell infusion (moment 2), and 100 days after transplantation (moment 3). In each moment, oral changes were assigned scores and classified as mild, moderate, and severe risks.

RESULTS:

The most frequent pathological conditions were gingivitis, pericoronitis in the third molar region, and ulcers at the third moment assessments. However, at moments 2 and 3, the most common disease was mucositis associated with toxicity from the drugs used in the immunosuppression.

CONCLUSION:

Mucositis accounted for the increased score and potential risk of clinical complications. Gingivitis, ulcers, and pericoronitis were other changes identified as potential risk factors for clinical complications.

Mucositis; Hematopoietic stem cell transplantation; Medical oncology

INTRODUÇÃO:

Pacientes submetidos a transplante de células hematopoiéticas recebem altas doses de quimioterapia e radioterapia que podem causar imunossupressão e doenças orais graves.

OBJETIVO:

Apresentar um protocolo de avaliação de doenças orais antes e após transplante de células hematopoiéticas.

MÉTODO:

Estudo clínico prospectivo de 65 pacientes com idade acima de 18 anos, com doenças hematológicas submetidas a transplante de células hematopoiéticas, divididos em dois grupos: A (transplante alogênico, 34 pacientes) e B (transplante autólogo). Foram realizadas três avaliações odontológicas: período antes do transplante (momento 1), uma semana (momento 2) e 100 dias após o transplante (momento 3). Em cada momento as alterações orais foram pontuadas e classificadas como leve, moderada e grave.

RESULTADOS:

As alterações orais mais frequentes foram: gengivite, pericoronite do terceiro molar e úlceras. Entretanto nos momentos dois e três a principal doença foi a mucosite associada a toxicidades das drogas usadas na imunossupressão.

CONCLUSÃO:

Mucosite foi principal alteração, com a pontuação mais alta e com maior risco de complicações. Gengivites, úlceras e pericoronites foram outras alterações com risco menor de complicações.

Mucosite; Sistema hematopoético; Oncologia

Introduction

Hematopoietic stem cell transplantation (HSCT) is the replacement of a diseased or deficient bone marrow by normal cells, with the aim of reconstituting the marrow and providing immune system control. It is classified as autologous when bone marrow precursor cells come from the patient, and as allogeneic, when the cells come from another person (donor), who may or may not be related to the recipient.¹1. Dulley F, Saboya R. Transplante de medula óssea. In: Trans- plante de órgãos e tecidos. 2nd ed. São Paulo: Ed. Segmento Farma; 2006. p. 849-50. ^and ²2. Schubert MM. Oral complications. In: Thomas ED, Blume KG, Forman SJ, editors. Hematopoietic cell transplantation. Black- well Science; 1999. p. 751-65.

Patients who will undergo HSCT are submitted to high doses of chemotherapy and radiation therapy to eradicate the underlying disease, which induces an intense immunosuppression period known as the conditioning phase. This period is characterized by possible tissue damage and infections due to immunosuppressive drug toxicity.³3. McGuire DB, Altomont V, Peterson DE. Patterns of mucositis and pain in patients receiving preparative chemotherapy and bone marrow transplantation. Oncol Nurs Forum. 1993;20:1493-502. ^, ⁴4. Dahllöf G, Bagessund M, Ringdén O. Impact of conditioning regi- mens on salivary function, caries-associated microorganisms and dental caries in children after bone marrow transplan- tation. A 4-years longitudinal study. Bone Marrow Transplant. 1997;20:479-83. ^and ⁵5. Blijlevens N, Schwenkglenks M, Bacon P, D'addio A, Ein- sele H, Maertens J, et al. Prospective oral mucositis audit: oral mucositis in patients receiving high-dose melphalan or BEAM conditioning chemotherapy - European blood and mar- row transplantation mucositis advisory group. J Clin Oncol. 2008;26:1519-25.

Mucositis is one of the most common oral tissue lesions described in these immunosuppressed patients, caused by the toxicity of these drugs; it results in a fragility of the oral mucosa with decreased numbers of basal cells, and even the onset of ulcerations.⁶6. Sonis ST. Mucositis as a biological process a new hypothesis for the development of chemotherapy-induced stomatotoxicity. Oral Oncol. 1998;34:39-43. ^, ⁷7. Sonis ST, Castello KA. A data base for mucositis induced by cancer chemotherapy. Oral Oncol. 1995;315:258-60. ^and ⁸8. López -Castanõ F, Onate-Sanchez RE, Roldán-Chicano R, Cabrerizo-Merino MC. Measurement of secondary mucositis to oncohematologic treatment by means of different scale. Med Oral Cir Bucal. 2005;10:412-21. It is considered the most important oral cavity complication in patients undergoing bone marrow suppression, and is also the most common, with an incidence of 90%.⁹9. Epstein JB, Schubert MM. Oral mucositis in myelossupres- sive CA therapy. Oral Surg Oral Med Pathol Radiol Endod. 1999;88:273-6. ^and ¹⁰10. Puyal M, Jimenéz C, Chimenos E, Lópes J, Juliá A. Protocolo de estudio y tratamiento de la mucositis bucal in los pacientes com hematopatias malignas. Med Oral. 2003;8:10-8. Kolbinson et al.¹¹11. Kolbinson DA, Shubert MM, Flournoy N, Truelove EL. Early oral changes following bone marrow transplantation. Oral Surg Oral Med Pathol. 1988;66:130-8. described early changes in the oral mucosa such as erythema, ulceration, and epithelial pseudomembrane formation that appear between five and seven days after the onset of chemotherapy and improve after three weeks.

These lesions represent a significant risk factor for systemic infections, particularly in patients with neutropenia, and 20-50% of cases of septicemia originate from the oral cavity.¹²12. Sonis ST, ODonnell KE, Popat R, Bragdon C, Phelan S, Cocks D, et al. The relationship between mucosal cyclooxigenase-2 (COX- 2) expression and experimental radiation induced mucositis. Oral Oncol. 2004;40:170-6. ^, ¹³13. Nucci M, Spector N, Bueno AP, Solzac C, Perecmanis T, Bacha PC, et al. Risk factors and attributable mortality associated with superinfections in neutropenic patients with cancer. Clin Infect Dis. 1995;24:575-9. ^and ¹⁴14. Porak D. Factors influencing the severity of radiation skin and oral mucosal reactions: development of a conceptual frame- work. Eur J Cancer Care (Engl). 2002;1:33-43. For Puyal et al.,¹⁰10. Puyal M, Jimenéz C, Chimenos E, Lópes J, Juliá A. Protocolo de estudio y tratamiento de la mucositis bucal in los pacientes com hematopatias malignas. Med Oral. 2003;8:10-8. Köstler et al.,¹⁵15. Köstler WJ, Hejna M, Wenzel C, Zielinski CC. Oral mucositis complications chemotherapy and or radiotherapy: options for prevention and treatment. Cancer J Clin. 2001;51:290-315. and Yamagata et al.,¹⁶16. Yamagata K, Onizawa K, Yanagawa T, Hasegawa Y, Kogina H, Nakasawa T, et al. A prospective study to evaluate a new dental management protocol before hematopoietic stem cell trans- plantation. Bone Marrow Transplant. 2006;38:237-42. the rates of occurrence of oral lesions varied, depending on the type of underlying disease, the treatment used and oral status before conditioning for transplantation, and reflected mainly pre-existing oral conditions.

Lesions such as root fragments, periodontal pockets, periapical lesions, and removable dentures are considered reservoirs of opportunistic pathogens that can trigger infections during immunosuppression.⁹9. Epstein JB, Schubert MM. Oral mucositis in myelossupres- sive CA therapy. Oral Surg Oral Med Pathol Radiol Endod. 1999;88:273-6. ^, ¹⁷17. Neville BW, Damm DD, Allen CM, Bouquot JE. Doenças imuno- logicamente mediadas e suas avaliações. In: Patologia oral & maxilofacial. 2nd ed. Rio de Janeiro: Ed. Guanabara- Koogan; 2004. p. 658-66. ^, ¹⁸18. Barker GJ. Current practices in the oral management of the patients undergoing chemotherapy or bone marrow transplan- tation. Support Care Cancer. 1999;7:17-20. ^and ¹⁹19. Silva L, Filho IB. Avaliação dos fatores de risco para mucosite oral em um grupo de pacientes sob terapia de transplante de medula. Acta Otorrinolaringol. 2007;25:104-11.

These reports indicate that the prevention of oral disease prior to HSCT is extremely important and that oral diseases should be treated before transplantation to eliminate potential risk factors for systemic infections.⁷7. Sonis ST, Castello KA. A data base for mucositis induced by cancer chemotherapy. Oral Oncol. 1995;315:258-60. ^, ²⁰20. Pico JL, Ávila-Garavito A. Mucositis: its occurrence, conse- quences and treatment in the oncology setting. Oncologist. 1998;3:446-51. ^, ²¹21. Heimdahl A, Mattisson T, Dahllof G, Lonnquist B, Ringden O. The oral cavity as a entry for early infections in patients treated with bone marrow transplantation. Oral Surg Med Pathol. 1989;68:711-6. ^and ²²22. Dreizen S, Mc Credie KB, Bodey GP, Keating MJ. Quantitative analysis of the oral complications of anti-leukemia chemother- apy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3. Dreizen et al.²²22. Dreizen S, Mc Credie KB, Bodey GP, Keating MJ. Quantitative analysis of the oral complications of anti-leukemia chemother- apy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3. reported that 30-50% of patients undergoing chemotherapy for oncologic treatment develop oral alterations or lesions, and that incidence can be significantly reduced by prior oral intervention. However, we found few studies in the literature, except those for mucositis, which attempted to quantify oral alterations that occur in patients undergoing bone marrow transplantation. When the authors, applied a score to the condition, they eliminated the subjective nature of the potential of these alterations for clinical complications.³3. McGuire DB, Altomont V, Peterson DE. Patterns of mucositis and pain in patients receiving preparative chemotherapy and bone marrow transplantation. Oncol Nurs Forum. 1993;20:1493-502. ^, ⁷7. Sonis ST, Castello KA. A data base for mucositis induced by cancer chemotherapy. Oral Oncol. 1995;315:258-60. ^, ⁸8. López -Castanõ F, Onate-Sanchez RE, Roldán-Chicano R, Cabrerizo-Merino MC. Measurement of secondary mucositis to oncohematologic treatment by means of different scale. Med Oral Cir Bucal. 2005;10:412-21. ^, ²³23. Sonis ST, Kuns A. Impact of improved dental services on the frequency of oral complications of cancer therapy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3. ^, ²⁴24. Parulekan W, Mackenzie R, Bjarnason G, Jordan RG. Scoring oral mucositis. Oral Oncol. 1998;34:63-71. ^, ²⁵25. Dodd MJ, Dibble S, Miaskowski C, Paul S, Cho M, Mcphael L, et al. A comparison of the affective state and quality of life of chemotherapy patients who do and do not develop chemotherapy-induced oral mucositis. J Pain Sym Manag. 2001;21:498-505. ^, ²⁶26. Rambrg P, Lindhe J, Dahen G, Volpe AR. The influence of gingiva inflammation on a new plaque formation. J Clin Periodontol. 1994;21:51-6. ^, ²⁷27. Daly CG, Highfield JE. Effect of localized experimental gingivitis on early supragingival plaque accumulation. J Clin Periodontol. 1996;23:160-4. ^, ²⁸28. Shulman JD, River-Hidalgo F, Beach MM. Risks factors associated with denture stomatitis in the United States. J Oral Pathol Med. 2005;34:340-6. ^, ²⁹29. De Lima DC, Nakata GC, Balducci I, Almeida JD. Oral mani- festations of diabetes mellitus in complete denture wearers. J Prostet Dent. 2008;99:60-5. ^and ³⁰30. Schubert M, Sullivan KM. Recognition, incidence and man- agement of oral graft-versus-host disease. NCI Monagr. 1990;9:134-43. Thus, the objective of this research was to develop a standardized method for the quantitative evaluation of alterations or lesions of the oral cavity, and to identify the potential for clinical complications in patients submitted to HSCT.

Methods

The present study was a clinical, prospective, six-month longitudinal temporal cohort study, with a data collection period of 24 months, performed at a referral hospital. The study was approved by the local research Ethics Committee (No. 39/2007). A total of 65 patients aged > 18 years, of both genders, with or without hematological malignancies, who underwent HSCT and immunosuppression in the abovementioned period were included. Patients were grouped according to the type of HSCT: group A (allogeneic), 34 patients; and group B (autologous), 31 patients. Initially, all answered a questionnaire, which contained information on oral health and oral hygiene habits. Subsequently, the patients were evaluated according to the status of the oral cavity at 20 days, on average, before conditioning and HSCT (moment 1). The second evaluation was carried out in the first week after transplantation (moment 2), and the last evaluation 100 days after HSCT (moment 3).

At the evaluation moments (1, 2, and 3) scores were given to the different alterations found in the oral cavity, according to the proposed dental standardization (Table 1). The score given to the oral alterations was based on previous work, which gave greater or lesser degree of importance to the histopathological alterations of the oral cavity.³3. McGuire DB, Altomont V, Peterson DE. Patterns of mucositis and pain in patients receiving preparative chemotherapy and bone marrow transplantation. Oncol Nurs Forum. 1993;20:1493-502. ^, ⁷7. Sonis ST, Castello KA. A data base for mucositis induced by cancer chemotherapy. Oral Oncol. 1995;315:258-60. ^, ⁸8. López -Castanõ F, Onate-Sanchez RE, Roldán-Chicano R, Cabrerizo-Merino MC. Measurement of secondary mucositis to oncohematologic treatment by means of different scale. Med Oral Cir Bucal. 2005;10:412-21. ^, ⁹9. Epstein JB, Schubert MM. Oral mucositis in myelossupres- sive CA therapy. Oral Surg Oral Med Pathol Radiol Endod. 1999;88:273-6. ^, ¹⁰10. Puyal M, Jimenéz C, Chimenos E, Lópes J, Juliá A. Protocolo de estudio y tratamiento de la mucositis bucal in los pacientes com hematopatias malignas. Med Oral. 2003;8:10-8. ^, ¹⁴14. Porak D. Factors influencing the severity of radiation skin and oral mucosal reactions: development of a conceptual frame- work. Eur J Cancer Care (Engl). 2002;1:33-43. ^and ²⁴24. Parulekan W, Mackenzie R, Bjarnason G, Jordan RG. Scoring oral mucositis. Oral Oncol. 1998;34:63-71. The risk classification and degrees of toxicity were based on the work of Porak,¹⁴14. Porak D. Factors influencing the severity of radiation skin and oral mucosal reactions: development of a conceptual frame- work. Eur J Cancer Care (Engl). 2002;1:33-43.Dreizen et al.,²²22. Dreizen S, Mc Credie KB, Bodey GP, Keating MJ. Quantitative analysis of the oral complications of anti-leukemia chemother- apy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3. and Parulekan et al.²⁴24. Parulekan W, Mackenzie R, Bjarnason G, Jordan RG. Scoring oral mucositis. Oral Oncol. 1998;34:63-71. In moment 1, patients were classified according to the risk for complications: mild (up to 15 points), moderate (16-30 points), and severe (31-50 points) risk. In moments 2 and 3, the degrees of toxicity were classified as follows: mild (15 points), moderate (16-30 points), and severe (31-50 points; Table 1).

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Table 1
Data standardization form with scores related to changes in the oral cavity.

Evaluation results were compared among themselves and between groups. For the variables gender, age, disease, drugs for conditioning, cell source, and type of transplantation, the chi-squared or Fisher's exact test were used for comparison of the groups. For the variables dental caries, gingival pockets, tooth mobility, tooth extractions, dentures, orthodontic devices, oral lesions, bacterial, viral, fungal infections, and mucositis, the Mann-Whitney test was used. Comparison between groups at each evaluation was performed using Friedman's test and comparison of moments within each group was performed using Fisher's test. The level of significance was set at 5% (p < 0.05).

Results

After the assessment of oral alterations, the classification of risks and toxicity of patients was performed by summation of the scores (Table 2, Table 3 and Table 4). In the first assessment, before conditioning, most patients received a mild risk classification in both groups. The only patient classified as having moderate risk had gingival pockets > 6 mm and tooth mobility; that patient's score was > 16 (Table 5).

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Table 2
Distribution of oral abnormalities observed in subjects from group A.

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Table 3
Distribution of oral abnormalities observed in subjects from group B.

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Table 4
Patient distribution by group and grade of mucositis.

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Table 5
Distribution of patients by transplantation group and risk at moment 1, p = 0.34.

In the second evaluation, of the 34 assessed patients in group A, 18 had mild toxicity, 15 moderate, and one patient had severe toxicity. In group B, of the 31 patients assessed, 19 had mild toxicity, 11 moderate, and one patient had severe toxicity (Table 6). As it can be observed, the risk and toxicity classification in both groups were performed according to the presence of mucositis and its degree of severity.

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Table 6
Distribution of patients by transplantation group and toxicity at moment 2.

In the third evaluation, as a result of deaths, 28 patients were assessed in group A and 30 patients in group B. All but one patient had mild toxicity in this assessment, and one patient persisted with severe toxicity (Table 7).

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Table 7
Distribution of patients according to group and toxicity at moment 3.

No statistical differences were observed regarding the scores in both groups A and B, for the variables dental caries, gingival pockets, tooth mobility, tooth extraction indication, dentures, and orthodontics in the three moments (Table 2 and Table 3). Comparing the moments of assessment within the groups, it was observed that there was no statistically significant increase in oral mucosal lesions over time within group A (p = 0.039). However, a statistically significant difference was observed when comparing moment 2 of groups A versus B, as mucositis was observed in 100% of individuals in both groups at these moments ( Table 2 and Table 3).

Discussion

HSCT is a widely used therapeutic technique, aiming to cure oncologic patients and to provide disease control.¹1. Dulley F, Saboya R. Transplante de medula óssea. In: Trans- plante de órgãos e tecidos. 2nd ed. São Paulo: Ed. Segmento Farma; 2006. p. 849-50. However, conditioning with chemotherapy drugs can result in several oral and systemic alterations in immunosuppressed patients.³3. McGuire DB, Altomont V, Peterson DE. Patterns of mucositis and pain in patients receiving preparative chemotherapy and bone marrow transplantation. Oncol Nurs Forum. 1993;20:1493-502. ^, ⁴4. Dahllöf G, Bagessund M, Ringdén O. Impact of conditioning regi- mens on salivary function, caries-associated microorganisms and dental caries in children after bone marrow transplan- tation. A 4-years longitudinal study. Bone Marrow Transplant. 1997;20:479-83. ^, ⁵5. Blijlevens N, Schwenkglenks M, Bacon P, D'addio A, Ein- sele H, Maertens J, et al. Prospective oral mucositis audit: oral mucositis in patients receiving high-dose melphalan or BEAM conditioning chemotherapy - European blood and mar- row transplantation mucositis advisory group. J Clin Oncol. 2008;26:1519-25. ^and ⁶6. Sonis ST. Mucositis as a biological process a new hypothesis for the development of chemotherapy-induced stomatotoxicity. Oral Oncol. 1998;34:39-43. These manifestations can increase the length of hospital stay, increase treatment costs, and directly affect the quality and quantity of life of these patients.²⁵25. Dodd MJ, Dibble S, Miaskowski C, Paul S, Cho M, Mcphael L, et al. A comparison of the affective state and quality of life of chemotherapy patients who do and do not develop chemotherapy-induced oral mucositis. J Pain Sym Manag. 2001;21:498-505.

In the autologous HSCT, comorbidities occur most often due to the underlying disease activity, whereas in allogeneic HSCT, they are due to systemic complications and the graft versus host reaction itself.¹1. Dulley F, Saboya R. Transplante de medula óssea. In: Trans- plante de órgãos e tecidos. 2nd ed. São Paulo: Ed. Segmento Farma; 2006. p. 849-50. ^, ²2. Schubert MM. Oral complications. In: Thomas ED, Blume KG, Forman SJ, editors. Hematopoietic cell transplantation. Black- well Science; 1999. p. 751-65. ^, ¹⁷17. Neville BW, Damm DD, Allen CM, Bouquot JE. Doenças imuno- logicamente mediadas e suas avaliações. In: Patologia oral & maxilofacial. 2nd ed. Rio de Janeiro: Ed. Guanabara- Koogan; 2004. p. 658-66. ^and ³⁰30. Schubert M, Sullivan KM. Recognition, incidence and man- agement of oral graft-versus-host disease. NCI Monagr. 1990;9:134-43. The intense immunosuppression predisposes transplanted patients to severe infections that can occur at any time of transplantation, can be caused by different etiological agents such as bacteria, fungi, viruses, or parasites.¹³13. Nucci M, Spector N, Bueno AP, Solzac C, Perecmanis T, Bacha PC, et al. Risk factors and attributable mortality associated with superinfections in neutropenic patients with cancer. Clin Infect Dis. 1995;24:575-9. ^and ²¹21. Heimdahl A, Mattisson T, Dahllof G, Lonnquist B, Ringden O. The oral cavity as a entry for early infections in patients treated with bone marrow transplantation. Oral Surg Med Pathol. 1989;68:711-6.

Establishing risk factors by assessing the status of the oral cavity and systemic complications of HSCT, and by assigning scores to the alterations at different times of the clinical follow-up of patients submitted to immunoexpression might facilitate the identification of individuals who would potentially have more clinical complications.⁸8. López -Castanõ F, Onate-Sanchez RE, Roldán-Chicano R, Cabrerizo-Merino MC. Measurement of secondary mucositis to oncohematologic treatment by means of different scale. Med Oral Cir Bucal. 2005;10:412-21. ^and ¹⁶16. Yamagata K, Onizawa K, Yanagawa T, Hasegawa Y, Kogina H, Nakasawa T, et al. A prospective study to evaluate a new dental management protocol before hematopoietic stem cell trans- plantation. Bone Marrow Transplant. 2006;38:237-42. A quantitative analysis using scores eliminates the subjective nature of the observations.²⁴24. Parulekan W, Mackenzie R, Bjarnason G, Jordan RG. Scoring oral mucositis. Oral Oncol. 1998;34:63-71. In the present study, the development and utilization of scores for oral alterations were based on previous studies that sought to associate, through scores or degrees of intensity, what changes or oral diseases associated with transplantation would, in theory, have greater potential to be associated with clinical complications.¹⁴14. Porak D. Factors influencing the severity of radiation skin and oral mucosal reactions: development of a conceptual frame- work. Eur J Cancer Care (Engl). 2002;1:33-43. ^, ¹⁶16. Yamagata K, Onizawa K, Yanagawa T, Hasegawa Y, Kogina H, Nakasawa T, et al. A prospective study to evaluate a new dental management protocol before hematopoietic stem cell trans- plantation. Bone Marrow Transplant. 2006;38:237-42. ^, ¹⁹19. Silva L, Filho IB. Avaliação dos fatores de risco para mucosite oral em um grupo de pacientes sob terapia de transplante de medula. Acta Otorrinolaringol. 2007;25:104-11. ^, ²²22. Dreizen S, Mc Credie KB, Bodey GP, Keating MJ. Quantitative analysis of the oral complications of anti-leukemia chemother- apy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3. ^and ²⁴24. Parulekan W, Mackenzie R, Bjarnason G, Jordan RG. Scoring oral mucositis. Oral Oncol. 1998;34:63-71.

The creation of tables and dental records was made based on the following variables: dental caries, gingival pockets, tooth mobility, root fragments, tooth extraction indication, use of dentures, orthodontic devices, and oral lesions.

Alterations also included the specific complications of HSCT, such as the occurrence of bacterial, fungal and viral infections, as well as the degree of mucositis.⁸8. López -Castanõ F, Onate-Sanchez RE, Roldán-Chicano R, Cabrerizo-Merino MC. Measurement of secondary mucositis to oncohematologic treatment by means of different scale. Med Oral Cir Bucal. 2005;10:412-21. ^, ¹⁴14. Porak D. Factors influencing the severity of radiation skin and oral mucosal reactions: development of a conceptual frame- work. Eur J Cancer Care (Engl). 2002;1:33-43. ^and ²²22. Dreizen S, Mc Credie KB, Bodey GP, Keating MJ. Quantitative analysis of the oral complications of anti-leukemia chemother- apy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3.

With respect to dental caries, the present data and those in the literature showed no significant increase in new dental caries in patients in the post-transplantation period and, as they are not relevant to HSCT complications, they have minimal score.

The gingival status and tooth mobility have a potential risk factor for complications, especially periodontal pockets greater than 6 mm.²⁶26. Rambrg P, Lindhe J, Dahen G, Volpe AR. The influence of gingiva inflammation on a new plaque formation. J Clin Periodontol. 1994;21:51-6. ^and ²⁷27. Daly CG, Highfield JE. Effect of localized experimental gingivitis on early supragingival plaque accumulation. J Clin Periodontol. 1996;23:160-4. Gingival pockets of this size favor greater accumulation of bacteria and necrotic tissue, and increase the risks for dental and oral disease; therefore, they received scores of up to 15, with intermediate values between dental caries and mucositis.

In both groups of the present study, only one patient had larger gingival pockets, ranging from 5 mm to 8 mm, and was classified at moment 1 as moderate risk and at moments 2 and 3 as severe toxicity, due to the presence of deep gingival pockets.

Another common observation, in approximately 80% of the patients, was gingival hyperemia, probably due to toxic reactions to drugs used during conditioning. Another likely cause is oral mucosa sensitization due to antiseptic mouthwash (chlorhexidine) used in oral hygiene. Patients do not brush their teeth for fear that trauma caused by the brush can cause bleeding, due to thrombocytopenia.

However, the lack of brushing can result in an increase in bacterial plaque, causing gingivitis, such as that seen in individuals at moment 2 in both groups, with a consequently greater risk of bleeding. When there is gingival inflammation, plaque can form more rapidly in those sites than in non-inflamed ones and thus, mouthwash would be less effective for oral hygiene. However, in the present sample, these alterations were barely observed, which was attributed to more effective actions before transplantation by the treating institution.¹1. Dulley F, Saboya R. Transplante de medula óssea. In: Trans- plante de órgãos e tecidos. 2nd ed. São Paulo: Ed. Segmento Farma; 2006. p. 849-50. ^, ²2. Schubert MM. Oral complications. In: Thomas ED, Blume KG, Forman SJ, editors. Hematopoietic cell transplantation. Black- well Science; 1999. p. 751-65. ^, ¹⁰10. Puyal M, Jimenéz C, Chimenos E, Lópes J, Juliá A. Protocolo de estudio y tratamiento de la mucositis bucal in los pacientes com hematopatias malignas. Med Oral. 2003;8:10-8. ^, ¹⁶16. Yamagata K, Onizawa K, Yanagawa T, Hasegawa Y, Kogina H, Nakasawa T, et al. A prospective study to evaluate a new dental management protocol before hematopoietic stem cell trans- plantation. Bone Marrow Transplant. 2006;38:237-42. ^and ¹⁷17. Neville BW, Damm DD, Allen CM, Bouquot JE. Doenças imuno- logicamente mediadas e suas avaliações. In: Patologia oral & maxilofacial. 2nd ed. Rio de Janeiro: Ed. Guanabara- Koogan; 2004. p. 658-66.

Findings such as tooth extractions and semi-impacted third molars with a history of pericoronitis are mentioned in the literature as having little potential as source of opportunistic pathogens and, as they were seldom observed, they were not scored.²¹21. Heimdahl A, Mattisson T, Dahllof G, Lonnquist B, Ringden O. The oral cavity as a entry for early infections in patients treated with bone marrow transplantation. Oral Surg Med Pathol. 1989;68:711-6. ^, ²²22. Dreizen S, Mc Credie KB, Bodey GP, Keating MJ. Quantitative analysis of the oral complications of anti-leukemia chemother- apy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3. ^and ²³23. Sonis ST, Kuns A. Impact of improved dental services on the frequency of oral complications of cancer therapy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3.

Semi-impacted third molars were observed in eight patients from group A and nine from group B. At moment 2, together with mucositis lesions, there was formation of plaque and gingiva overlying the tooth. For this type of finding, and for prostheses and orthodontic devices, 1 point was scored. Shulman et al.²⁸28. Shulman JD, River-Hidalgo F, Beach MM. Risks factors associated with denture stomatitis in the United States. J Oral Pathol Med. 2005;34:340-6. reported that orthodontic devices and dentures are risk factors for stomatitis.

Even with the knowledge of this report of possible health risks for individuals wearing prostheses, it was not possible to establish statistically significant data correlating them with oral alterations.²⁹29. De Lima DC, Nakata GC, Balducci I, Almeida JD. Oral mani- festations of diabetes mellitus in complete denture wearers. J Prostet Dent. 2008;99:60-5. But since we knew that the oral cavity is the gateway of infections in patients undergoing immunosuppression for bone marrow transplantation and that the use of orthodontic devices and dentures can potentiate them, we asked our patients not to wear them, if possible.²¹21. Heimdahl A, Mattisson T, Dahllof G, Lonnquist B, Ringden O. The oral cavity as a entry for early infections in patients treated with bone marrow transplantation. Oral Surg Med Pathol. 1989;68:711-6. These recommendations were made before the first evaluation, and were the reasons for the paucity of alterations at moment 1. Although that was not the purpose of this study, we demonstrated the importance of prevention and treatment of oral diseases to lessen the risk of clinical complications in immunosuppressed individuals.⁸8. López -Castanõ F, Onate-Sanchez RE, Roldán-Chicano R, Cabrerizo-Merino MC. Measurement of secondary mucositis to oncohematologic treatment by means of different scale. Med Oral Cir Bucal. 2005;10:412-21. ^and ²¹21. Heimdahl A, Mattisson T, Dahllof G, Lonnquist B, Ringden O. The oral cavity as a entry for early infections in patients treated with bone marrow transplantation. Oral Surg Med Pathol. 1989;68:711-6. This was also the opinion of Sonis and Kuns,²³23. Sonis ST, Kuns A. Impact of improved dental services on the frequency of oral complications of cancer therapy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3. who showed a decrease in these complications when such care was performed.

Some non-infectious oral lesions, such as oral leukoplakia, gingival hyperplasia, and others that are seldom described by other authors, also infrequently were observed by the present authors. Oral lesions similar to hemorrhagic lesions that were difficult to characterize, but did not evoke clinical complaints were observed in 17 patients from group A and eight patients from group B at moment 2, caused perhaps by thrombocytopenia; these were resolved in moment 3.

The literature documents that mucositis is unquestionably the oral alteration that is the main risk factor for the systemic infections that occur in between 20% and 50% of HSCT patients, most prevalent in those with associated neutropenia.³3. McGuire DB, Altomont V, Peterson DE. Patterns of mucositis and pain in patients receiving preparative chemotherapy and bone marrow transplantation. Oncol Nurs Forum. 1993;20:1493-502. ^, ⁵5. Blijlevens N, Schwenkglenks M, Bacon P, D'addio A, Ein- sele H, Maertens J, et al. Prospective oral mucositis audit: oral mucositis in patients receiving high-dose melphalan or BEAM conditioning chemotherapy - European blood and mar- row transplantation mucositis advisory group. J Clin Oncol. 2008;26:1519-25. ^, ⁶6. Sonis ST. Mucositis as a biological process a new hypothesis for the development of chemotherapy-induced stomatotoxicity. Oral Oncol. 1998;34:39-43. ^, ⁷7. Sonis ST, Castello KA. A data base for mucositis induced by cancer chemotherapy. Oral Oncol. 1995;315:258-60. ^, ⁸8. López -Castanõ F, Onate-Sanchez RE, Roldán-Chicano R, Cabrerizo-Merino MC. Measurement of secondary mucositis to oncohematologic treatment by means of different scale. Med Oral Cir Bucal. 2005;10:412-21. ^, ⁹9. Epstein JB, Schubert MM. Oral mucositis in myelossupres- sive CA therapy. Oral Surg Oral Med Pathol Radiol Endod. 1999;88:273-6. ^, ¹⁰10. Puyal M, Jimenéz C, Chimenos E, Lópes J, Juliá A. Protocolo de estudio y tratamiento de la mucositis bucal in los pacientes com hematopatias malignas. Med Oral. 2003;8:10-8. ^, ¹⁹19. Silva L, Filho IB. Avaliação dos fatores de risco para mucosite oral em um grupo de pacientes sob terapia de transplante de medula. Acta Otorrinolaringol. 2007;25:104-11. ^, ²⁰20. Pico JL, Ávila-Garavito A. Mucositis: its occurrence, conse- quences and treatment in the oncology setting. Oncologist. 1998;3:446-51. ^and ²¹21. Heimdahl A, Mattisson T, Dahllof G, Lonnquist B, Ringden O. The oral cavity as a entry for early infections in patients treated with bone marrow transplantation. Oral Surg Med Pathol. 1989;68:711-6. The intensity of mucositis can vary depending on the underlying disease and the type of transplantation, as well as the oral status before and during immunosuppression.¹¹11. Kolbinson DA, Shubert MM, Flournoy N, Truelove EL. Early oral changes following bone marrow transplantation. Oral Surg Oral Med Pathol. 1988;66:130-8. ^, ¹⁴14. Porak D. Factors influencing the severity of radiation skin and oral mucosal reactions: development of a conceptual frame- work. Eur J Cancer Care (Engl). 2002;1:33-43. ^and ¹⁵15. Köstler WJ, Hejna M, Wenzel C, Zielinski CC. Oral mucositis complications chemotherapy and or radiotherapy: options for prevention and treatment. Cancer J Clin. 2001;51:290-315.

In the present study, the incidence of mucositis was 100% in the second evaluation, at moment 2, for both group A and group B patients. The risk association of moment 2 and mucositis was significant. Both groups showed an association of the risk classification and/or toxicity (mild, moderate, severe, and very severe) with the onset of mucositis and degrees of intensity. Most patients were classified as having mild risk, but those who developed mucositis were classified as having moderate or severe risk.

These patients also had oral lesions, more often on the tongue and labial mucosa, characterized as erythema of the oral mucosa, lichen planus, generalized erosions, ulcerations, and xerostomia.³⁰30. Schubert M, Sullivan KM. Recognition, incidence and man- agement of oral graft-versus-host disease. NCI Monagr. 1990;9:134-43.

Some authors reported that this is due to low oral food intake, because of pain caused by these lesions.¹⁸18. Barker GJ. Current practices in the oral management of the patients undergoing chemotherapy or bone marrow transplan- tation. Support Care Cancer. 1999;7:17-20. ^, ²¹21. Heimdahl A, Mattisson T, Dahllof G, Lonnquist B, Ringden O. The oral cavity as a entry for early infections in patients treated with bone marrow transplantation. Oral Surg Med Pathol. 1989;68:711-6. ^and ²⁵25. Dodd MJ, Dibble S, Miaskowski C, Paul S, Cho M, Mcphael L, et al. A comparison of the affective state and quality of life of chemotherapy patients who do and do not develop chemotherapy-induced oral mucositis. J Pain Sym Manag. 2001;21:498-505. In the present study, this observation was more evident, as 15 patients from group B required the introduction of parenteral nutrition. In this group of patients, the authors observed dysphagia, anorexia, and rapid weight loss soon after transplantation, as early as moment 2 of the evaluation.

We did not observe other infections, such as those caused by anaerobic organisms in our study probably due to preventive measures with oral fluconazole and nystatin, as well as the use of antiseptic mouthwash, which are a standard procedure in all patients undergoing HSCT.¹⁰10. Puyal M, Jimenéz C, Chimenos E, Lópes J, Juliá A. Protocolo de estudio y tratamiento de la mucositis bucal in los pacientes com hematopatias malignas. Med Oral. 2003;8:10-8. ^, ¹⁴14. Porak D. Factors influencing the severity of radiation skin and oral mucosal reactions: development of a conceptual frame- work. Eur J Cancer Care (Engl). 2002;1:33-43. ^and ¹⁵15. Köstler WJ, Hejna M, Wenzel C, Zielinski CC. Oral mucositis complications chemotherapy and or radiotherapy: options for prevention and treatment. Cancer J Clin. 2001;51:290-315.

Undoubtedly, the most feared complication of bone marrow transplantation is death, that occurs in 15-20% of allogeneic transplantations and in 5% of autologous transplantations. Is this related to oral alterations? Death occurred in seven of the present patients, between moments 2 and 3 after transplantation. One of the deaths occurred in group B, from multiple-organ failure and veno-occlusive disease. In group A, six patients died. Of these, four died due to disease recurrence, one patient died due to pneumonia and respiratory failure, and one patient due to acute host-versus-graft disease and sepsis. In none of them were the causes associated with oral disease. Although mucositis is the main alteration responsible for the increase in clinical complications, especially infectious ones associated to conditioning toxicity, such lesions were not seen in these patients at the time of death, perhaps due to the dramatic moment experienced by patients and the medical staff.

Conclusion

We affirm that mucositis is the oral cavity alteration of greatest concern as a potential risk for complications in immunosuppressed patients. Other lesions, such as gingivitis and third-molar pericoronitis, considered as low-risk indicators in this study were also less relevant. This alterations became more evident when the mild, moderate and severe risk and toxicity scores were used to assess the clinical complications in immunossupressed individuals.

References

¹
Dulley F, Saboya R. Transplante de medula óssea. In: Trans- plante de órgãos e tecidos. 2nd ed. São Paulo: Ed. Segmento Farma; 2006. p. 849-50.
²
Schubert MM. Oral complications. In: Thomas ED, Blume KG, Forman SJ, editors. Hematopoietic cell transplantation. Black- well Science; 1999. p. 751-65.
³
McGuire DB, Altomont V, Peterson DE. Patterns of mucositis and pain in patients receiving preparative chemotherapy and bone marrow transplantation. Oncol Nurs Forum. 1993;20:1493-502.
⁴
Dahllöf G, Bagessund M, Ringdén O. Impact of conditioning regi- mens on salivary function, caries-associated microorganisms and dental caries in children after bone marrow transplan- tation. A 4-years longitudinal study. Bone Marrow Transplant. 1997;20:479-83.
⁵
Blijlevens N, Schwenkglenks M, Bacon P, D'addio A, Ein- sele H, Maertens J, et al. Prospective oral mucositis audit: oral mucositis in patients receiving high-dose melphalan or BEAM conditioning chemotherapy - European blood and mar- row transplantation mucositis advisory group. J Clin Oncol. 2008;26:1519-25.
⁶
Sonis ST. Mucositis as a biological process a new hypothesis for the development of chemotherapy-induced stomatotoxicity. Oral Oncol. 1998;34:39-43.
⁷
Sonis ST, Castello KA. A data base for mucositis induced by cancer chemotherapy. Oral Oncol. 1995;315:258-60.
⁸
López -Castanõ F, Onate-Sanchez RE, Roldán-Chicano R, Cabrerizo-Merino MC. Measurement of secondary mucositis to oncohematologic treatment by means of different scale. Med Oral Cir Bucal. 2005;10:412-21.
⁹
Epstein JB, Schubert MM. Oral mucositis in myelossupres- sive CA therapy. Oral Surg Oral Med Pathol Radiol Endod. 1999;88:273-6.
¹⁰
Puyal M, Jimenéz C, Chimenos E, Lópes J, Juliá A. Protocolo de estudio y tratamiento de la mucositis bucal in los pacientes com hematopatias malignas. Med Oral. 2003;8:10-8.
¹¹
Kolbinson DA, Shubert MM, Flournoy N, Truelove EL. Early oral changes following bone marrow transplantation. Oral Surg Oral Med Pathol. 1988;66:130-8.
¹²
Sonis ST, ODonnell KE, Popat R, Bragdon C, Phelan S, Cocks D, et al. The relationship between mucosal cyclooxigenase-2 (COX- 2) expression and experimental radiation induced mucositis. Oral Oncol. 2004;40:170-6.
¹³
Nucci M, Spector N, Bueno AP, Solzac C, Perecmanis T, Bacha PC, et al. Risk factors and attributable mortality associated with superinfections in neutropenic patients with cancer. Clin Infect Dis. 1995;24:575-9.
¹⁴
Porak D. Factors influencing the severity of radiation skin and oral mucosal reactions: development of a conceptual frame- work. Eur J Cancer Care (Engl). 2002;1:33-43.
¹⁵
Köstler WJ, Hejna M, Wenzel C, Zielinski CC. Oral mucositis complications chemotherapy and or radiotherapy: options for prevention and treatment. Cancer J Clin. 2001;51:290-315.
¹⁶
Yamagata K, Onizawa K, Yanagawa T, Hasegawa Y, Kogina H, Nakasawa T, et al. A prospective study to evaluate a new dental management protocol before hematopoietic stem cell trans- plantation. Bone Marrow Transplant. 2006;38:237-42.
¹⁷
Neville BW, Damm DD, Allen CM, Bouquot JE. Doenças imuno- logicamente mediadas e suas avaliações. In: Patologia oral & maxilofacial. 2nd ed. Rio de Janeiro: Ed. Guanabara- Koogan; 2004. p. 658-66.
¹⁸
Barker GJ. Current practices in the oral management of the patients undergoing chemotherapy or bone marrow transplan- tation. Support Care Cancer. 1999;7:17-20.
¹⁹
Silva L, Filho IB. Avaliação dos fatores de risco para mucosite oral em um grupo de pacientes sob terapia de transplante de medula. Acta Otorrinolaringol. 2007;25:104-11.
²⁰
Pico JL, Ávila-Garavito A. Mucositis: its occurrence, conse- quences and treatment in the oncology setting. Oncologist. 1998;3:446-51.
²¹
Heimdahl A, Mattisson T, Dahllof G, Lonnquist B, Ringden O. The oral cavity as a entry for early infections in patients treated with bone marrow transplantation. Oral Surg Med Pathol. 1989;68:711-6.
²²
Dreizen S, Mc Credie KB, Bodey GP, Keating MJ. Quantitative analysis of the oral complications of anti-leukemia chemother- apy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3.
²³
Sonis ST, Kuns A. Impact of improved dental services on the frequency of oral complications of cancer therapy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3.
²⁴
Parulekan W, Mackenzie R, Bjarnason G, Jordan RG. Scoring oral mucositis. Oral Oncol. 1998;34:63-71.
²⁵
Dodd MJ, Dibble S, Miaskowski C, Paul S, Cho M, Mcphael L, et al. A comparison of the affective state and quality of life of chemotherapy patients who do and do not develop chemotherapy-induced oral mucositis. J Pain Sym Manag. 2001;21:498-505.
²⁶
Rambrg P, Lindhe J, Dahen G, Volpe AR. The influence of gingiva inflammation on a new plaque formation. J Clin Periodontol. 1994;21:51-6.
²⁷
Daly CG, Highfield JE. Effect of localized experimental gingivitis on early supragingival plaque accumulation. J Clin Periodontol. 1996;23:160-4.
²⁸
Shulman JD, River-Hidalgo F, Beach MM. Risks factors associated with denture stomatitis in the United States. J Oral Pathol Med. 2005;34:340-6.
²⁹
De Lima DC, Nakata GC, Balducci I, Almeida JD. Oral mani- festations of diabetes mellitus in complete denture wearers. J Prostet Dent. 2008;99:60-5.
³⁰
Schubert M, Sullivan KM. Recognition, incidence and man- agement of oral graft-versus-host disease. NCI Monagr. 1990;9:134-43.

☆
Please cite this article as: Barrach RH, de Souza MP, da Silva DP, Lopez PS, Montovani JC. Oral changes in individuals undergoing hematopoietic stem cell transplantation. Braz J Otorhinolaryngol. 2015;81:141-7.

Publication Dates

Publication in this collection
Apr 2015

History

Received
05 Nov 2013
Accepted
27 Apr 2014

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] ¹
Dulley F, Saboya R. Transplante de medula óssea. In: Trans- plante de órgãos e tecidos. 2nd ed. São Paulo: Ed. Segmento Farma; 2006. p. 849-50.

[2] ²
Schubert MM. Oral complications. In: Thomas ED, Blume KG, Forman SJ, editors. Hematopoietic cell transplantation. Black- well Science; 1999. p. 751-65.

[3] ³
McGuire DB, Altomont V, Peterson DE. Patterns of mucositis and pain in patients receiving preparative chemotherapy and bone marrow transplantation. Oncol Nurs Forum. 1993;20:1493-502.

[4] ⁴
Dahllöf G, Bagessund M, Ringdén O. Impact of conditioning regi- mens on salivary function, caries-associated microorganisms and dental caries in children after bone marrow transplan- tation. A 4-years longitudinal study. Bone Marrow Transplant. 1997;20:479-83.

[5] ⁵
Blijlevens N, Schwenkglenks M, Bacon P, D'addio A, Ein- sele H, Maertens J, et al. Prospective oral mucositis audit: oral mucositis in patients receiving high-dose melphalan or BEAM conditioning chemotherapy - European blood and mar- row transplantation mucositis advisory group. J Clin Oncol. 2008;26:1519-25.

[6] ⁶
Sonis ST. Mucositis as a biological process a new hypothesis for the development of chemotherapy-induced stomatotoxicity. Oral Oncol. 1998;34:39-43.

[7] ⁷
Sonis ST, Castello KA. A data base for mucositis induced by cancer chemotherapy. Oral Oncol. 1995;315:258-60.

[8] ⁸
López -Castanõ F, Onate-Sanchez RE, Roldán-Chicano R, Cabrerizo-Merino MC. Measurement of secondary mucositis to oncohematologic treatment by means of different scale. Med Oral Cir Bucal. 2005;10:412-21.

[9] ⁹
Epstein JB, Schubert MM. Oral mucositis in myelossupres- sive CA therapy. Oral Surg Oral Med Pathol Radiol Endod. 1999;88:273-6.

[10] ¹⁰
Puyal M, Jimenéz C, Chimenos E, Lópes J, Juliá A. Protocolo de estudio y tratamiento de la mucositis bucal in los pacientes com hematopatias malignas. Med Oral. 2003;8:10-8.

[11] ¹¹
Kolbinson DA, Shubert MM, Flournoy N, Truelove EL. Early oral changes following bone marrow transplantation. Oral Surg Oral Med Pathol. 1988;66:130-8.

[12] ¹²
Sonis ST, ODonnell KE, Popat R, Bragdon C, Phelan S, Cocks D, et al. The relationship between mucosal cyclooxigenase-2 (COX- 2) expression and experimental radiation induced mucositis. Oral Oncol. 2004;40:170-6.

[13] ¹³
Nucci M, Spector N, Bueno AP, Solzac C, Perecmanis T, Bacha PC, et al. Risk factors and attributable mortality associated with superinfections in neutropenic patients with cancer. Clin Infect Dis. 1995;24:575-9.

[14] ¹⁴
Porak D. Factors influencing the severity of radiation skin and oral mucosal reactions: development of a conceptual frame- work. Eur J Cancer Care (Engl). 2002;1:33-43.

[15] ¹⁵
Köstler WJ, Hejna M, Wenzel C, Zielinski CC. Oral mucositis complications chemotherapy and or radiotherapy: options for prevention and treatment. Cancer J Clin. 2001;51:290-315.

[16] ¹⁶
Yamagata K, Onizawa K, Yanagawa T, Hasegawa Y, Kogina H, Nakasawa T, et al. A prospective study to evaluate a new dental management protocol before hematopoietic stem cell trans- plantation. Bone Marrow Transplant. 2006;38:237-42.

[17] ¹⁷
Neville BW, Damm DD, Allen CM, Bouquot JE. Doenças imuno- logicamente mediadas e suas avaliações. In: Patologia oral & maxilofacial. 2nd ed. Rio de Janeiro: Ed. Guanabara- Koogan; 2004. p. 658-66.

[18] ¹⁸
Barker GJ. Current practices in the oral management of the patients undergoing chemotherapy or bone marrow transplan- tation. Support Care Cancer. 1999;7:17-20.

[19] ¹⁹
Silva L, Filho IB. Avaliação dos fatores de risco para mucosite oral em um grupo de pacientes sob terapia de transplante de medula. Acta Otorrinolaringol. 2007;25:104-11.

[20] ²⁰
Pico JL, Ávila-Garavito A. Mucositis: its occurrence, conse- quences and treatment in the oncology setting. Oncologist. 1998;3:446-51.

[21] ²¹
Heimdahl A, Mattisson T, Dahllof G, Lonnquist B, Ringden O. The oral cavity as a entry for early infections in patients treated with bone marrow transplantation. Oral Surg Med Pathol. 1989;68:711-6.

[22] ²²
Dreizen S, Mc Credie KB, Bodey GP, Keating MJ. Quantitative analysis of the oral complications of anti-leukemia chemother- apy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3.

[23] ²³
Sonis ST, Kuns A. Impact of improved dental services on the frequency of oral complications of cancer therapy. Oral Surg Oral Med Oral Pathol. 1986;62:650-3.

[24] ²⁴
Parulekan W, Mackenzie R, Bjarnason G, Jordan RG. Scoring oral mucositis. Oral Oncol. 1998;34:63-71.

[25] ²⁵
Dodd MJ, Dibble S, Miaskowski C, Paul S, Cho M, Mcphael L, et al. A comparison of the affective state and quality of life of chemotherapy patients who do and do not develop chemotherapy-induced oral mucositis. J Pain Sym Manag. 2001;21:498-505.

[26] ²⁶
Rambrg P, Lindhe J, Dahen G, Volpe AR. The influence of gingiva inflammation on a new plaque formation. J Clin Periodontol. 1994;21:51-6.

[27] ²⁷
Daly CG, Highfield JE. Effect of localized experimental gingivitis on early supragingival plaque accumulation. J Clin Periodontol. 1996;23:160-4.

[28] ²⁸
Shulman JD, River-Hidalgo F, Beach MM. Risks factors associated with denture stomatitis in the United States. J Oral Pathol Med. 2005;34:340-6.

[29] ²⁹
De Lima DC, Nakata GC, Balducci I, Almeida JD. Oral mani- festations of diabetes mellitus in complete denture wearers. J Prostet Dent. 2008;99:60-5.

[30] ³⁰
Schubert M, Sullivan KM. Recognition, incidence and man- agement of oral graft-versus-host disease. NCI Monagr. 1990;9:134-43.

Oral alterations	Moment 1 n = 34	Moment 2 n = 34	Moment 3 n = 28
Tooth caries	n = 19 (59.4%)	n = 19 (59.4%)	n = 18 (66.7%)
Gingival pockets	n = 8 (25.0%)	n = 8 (25.8%)	n = 7 (25.9%)
Mobility	n = 5 (15.6%)	n = 6 (18.8%)	n = 5 (18.5%)
Tooth loss	n = 10 (31.2%)	n = 9 (28.1)	n = 8 (29.6%)
Prostheses	n = 14 (41.2%)	n = 14 (41.2%)	n = 10 (35.7%)
Orthodontics	0	0	0
Oral lesions	n = 8 (23.5%)	n = 16 (47.1%)	n = 7 (53.6%)
Infections	–	–	n = 2 (7.2%)
Mucositis	0	n = 34 (100%)	0

Oral alterations	Moment 1 n = 31	Moment 2 n = 31	Moment 3 n = 30
Tooth caries	8 (26.7%)	8 (26.7%)	7 (24.1%)
Gingival pockets	8 (26.6%)	8 (26.6%)	8 (27.6)
Mobility	9 (30%)	9 (30%)	9 (31.0%)
Tooth loss	9 (30%)	9 (30%)	8 (27.6%)
Prostheses	18 (54.8%)	18 (54.8%)	18 (54.8%)
Orthodontics	2 (6.7%)	2 (6.7%)	2 (6.7%)
Oral lesions	5 (16.1%)	7 (22.6%)	5 (16.7%)
Infections	0	0	0
Mucositis	0	31 (100%)	0

Grade of mucositis	Group
	A		B
	n	%	n	%
I	7	20.6	8	25.8
II	9	26.5	10	32.3
III	10	29.4	9	29.0
IV	8	23.5	4	12.9
Total	34	100.0	31	100.0

Risk at moment 1
	Mild		Moderate		Total
Group	n	%	n	%	n	%
A	33	97.1	1	2.9	34	100.0
B	31	100.0	–	0.0	31	100.0
Total	64	98.5	1	1.5	65	100.0

Grades of toxicity at moment 2
Group	Mild		Moderate		Severe
	n	%	n	%	n	%
A	18	52.9	15	44.2	1	2.9
B	19	61.3	11	35.5	1	3.2

Brasil

Brasil

Oral changes in individuals undergoing hematopoietic stem cell transplantation ^☆ ☆ Please cite this article as: Barrach RH, de Souza MP, da Silva DP, Lopez PS, Montovani JC. Oral changes in individuals undergoing hematopoietic stem cell transplantation. Braz J Otorhinolaryngol. 2015;81:141-7.

Abstracts

INTRODUCTION:

OBJECTIVE:

METHODS:

RESULTS:

CONCLUSION:

INTRODUÇÃO:

OBJETIVO:

MÉTODO:

RESULTADOS:

CONCLUSÃO:

Introduction

Methods

Results

Discussion

Conclusion

References

Publication Dates

History

Brasil

Brasil

Oral changes in individuals undergoing hematopoietic stem cell transplantation ☆ ☆ Please cite this article as: Barrach RH, de Souza MP, da Silva DP, Lopez PS, Montovani JC. Oral changes in individuals undergoing hematopoietic stem cell transplantation. Braz J Otorhinolaryngol. 2015;81:141-7.

Abstracts

INTRODUCTION:

OBJECTIVE:

METHODS:

RESULTS:

CONCLUSION:

INTRODUÇÃO:

OBJETIVO:

MÉTODO:

RESULTADOS:

CONCLUSÃO:

Introduction

Methods

Results

Discussion

Conclusion

References

Publication Dates

History

Oral changes in individuals undergoing hematopoietic stem cell transplantation ^☆ ☆ Please cite this article as: Barrach RH, de Souza MP, da Silva DP, Lopez PS, Montovani JC. Oral changes in individuals undergoing hematopoietic stem cell transplantation. Braz J Otorhinolaryngol. 2015;81:141-7.