Neutropenia in a Tertiary Hospital: Epidemiology and Culture Isolates. Fatma S Al Qahtani, MBBS, KSUF Path*

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Bahrain Medical Bulletin, Volume 30, No 1, March 2008 Neutropenia in a Tertiary Hospital: Epidemiology and Culture Isolates Fatma S Al Qahtani, MBBS, KSUF Path* Objective: To study the causes, severity, and the frequency of neutropenia. Design: Retrospective medical chart review of patients with neutropenic episodes. Setting: King Khalid University Hospital, Riyadh, Saudi Arabia. Method: Consecutive patients with a diagnosis of neutropenia were reviewed and analyzed between January 1995 and December 2006. Personal characteristics and absolute neutrophil counts were documented. Result: Ninety-seven patients, 39 males and 58 females, with 113 episodes comprised the study group. Mean age was 38 ± 24.8 years. Mean absolute neutrophil count was 1184 ± 396 cells/mm3. There were 88 (90.7%) with mild neutropenia and 9 (9.3%) had moderate neutropenia. An infective focus was identified in 75 (77.3%) patients. Patients with mild neutropenia were significantly younger compared to patients with moderate neutropenia (p=0.0185) and had foci of infection in 81.8% of cases. Moderate neutropenia was seen in cancer patients and in those receiving chemotherapy. Fever was present in 84.5% of patients, who were younger and with shorter duration of neutropenic episodes compared to those who did not have fever. However, mortality was significantly greater among non-febrile patients than those with febrile episodes were (p=0.0294). Conclusion: There is a need to consider a variety of factors such as age, sex, infectious foci, presence of fever and even the duration of neutropenia for initiation of appropriate management protocols. The absence of fever may mislead physicians regarding the severity of the condition. Bahrain Med Bull 2008; 30(1): Neutropenia is a hematological disorder characterized by an abnormally low number of neutrophil granulocytes. It is defined as an absolute neutrophil count of less than 1500 cells/mm 3 and can be graded as mild (1000-1500 cells/mm 3 ), moderate (500-1000 cells/mm 3 ), or severe (<500 cells/mm 3 ) 1. Neutropenia can develop in one or more conditions including decreased bone marrow production, the sequestering of neutrophils and increased destruction of neutrophils in the peripheral blood. Decreased production in the bone marrow is seen in hereditary disorders, cancer, use of certain medications 2-7. Increased destruction of neutrophils is seen in aplastic anemia, autoimmune disorders and chemotherapy 8-11. * Consultant Pathologist Department of Pathology 1

King Khalid University Hospital Riyadh, Saudi Arabia Neutropenia leads to an increased risk of infection. Neutropenia is classified according to the etiology as congenital or acquired, with the latter further defined according to the etiology or pathology 12. Neutropenia may be undetected and generally discovered when a patient has developed severe infections or sepsis. Patients usually present with fever, frequent infections, mouth ulcers, diarrhea, burning sensation when urinating, sore throat and shortness of breath or shaking chills. Recent studies on isolates from patients with febrile neutropenia showed Staphylococcus, Streptococcus viridans, Escherichia coli, Pseudomonas aeruginosa Mucor spp and Candida albicans as the common bacterial and fungal isolates 3,13-17. The estimated incidence of severe chronic neutropenia is approximately one case per 100,000 in the USA. Cyclic neutropenia is the rarest with an estimated frequency of one per million in the USA. Severe chronic neutropenia is most frequently encountered as a pediatric problem. However, clinical symptoms tend to diminish with increasing age. Morbidity usually involves infections during severe, prolonged episodes of neutropenia. Serious medical complications occur in 21% of patients with cancer and neutropenic fever. Neutropenia occurs more commonly in females than males and the elderly have a higher incidence rate than younger individuals 18-19. Mortality correlates with increased risk of severe and rapidly progressing infections caused by bacteria and fungi, thus, a rapid empirical antibiotic therapy should be administered at the onset of fever 3. This study was conducted to study the causes, severity, and the frequency of neutropenia. METHOD A retrospective review of medical files of all patients with neutropenia seen from January 1995 to December 2006 was performed. Diagnosis of neutropenia was confirmed from the doctor's diagnosis. Neutropenia patients were reviewed for personal characteristics, hospital course, history, neutropenia status, dates and duration of neutropenia, management and interventions. Absolute confidentiality of the patients vital information was maintained for ethical purposes. Ethical approval was not considered due to the retrospective nature of the study; neither personal interviews nor questionnaire requiring direct contact with patients were performed. Inclusion criterion: All patients diagnosed with neutropenia (no age and sex limitations) seen between January 1995 to December 2006 were included in the study. Exclusion criteria: Patients who were diagnosed with neutropenia but without available laboratory results and incomplete patients records were excluded from the study. RESULT A total of 97 patients, 39 (40.2%) males and 58 (59.8%) females were diagnosed with neutropenia. Mean age was 38 ± 24.8 years (range: 1 month to 92 years). There was a total 2

of 113 neutropenia episodes in 97 patients; 82 (84.5%) patients with a single neutropenia episode, 14 (14.4%) with 2 episodes and 1 (1%) patient with 3 episodes. Mean duration of neutropenia was 2.4 ± 1.3 days (range: 1-7 days). Mean hospital stay was 12 ± 14 days (range: 2-74 days). Mean absolute neutrophil count (ANC) was 1184 ± 396 cells/mm 3 (range: 800 1500 cells/mm 3 ). Eighty-eight (90.7%) patients had mild neutropenia and 9 (9.3%) had moderate degree of neutropenia according to WHO classification 1 (see Table 1). Table 1: Personal Characteristics of Neutropenic Patients (N=97) Sex distribution Males 39 (40.2%) Females 58 (59.8%) Age (mean ± SD) Duration of neutropenia (mean ± SD) Absolute neutrophil count (mean ± SD) Causes Infection 75 (77.3%) Malignancy 10 (10.3%) Prematurity 5 (5.2%) Other 7 (7.2%) Intracranial hematoma (4) ESRD* on hemodialysis (2) Myasthenia gravis (1) *end stage renal disease 38 ± 24.8 years (1 month-92 yrs) 2.4 ± 1.3 days (1-7 days) 1184 ± 396 cells/mm 3 (800-1500) An infective focus was seen in 75 (77.3%) patients, cancer patients on chemotherapy in 10 (10.3%), prematurity in 5 (5.2%) and other causes in 7 (7.2%) patients. No patient was seen with benign cyclic neutropenia. Eighteen patients (18.6%) required insertion of a catheter, 8 (8.2%) needed a ventilator and 2 patients (2.1%) had nasogastric tube (NGT) inserted. Fever was present in 82 (84.5%) patients. Patients with mild neutropenia were significantly younger (mean of 30.67 ± 25.3 years) compared to those with moderate neutropenia (mean of 51.33 ± 15.4 years) (p=0.0185). Positive blood culture findings were similar in both mild and moderate neutropenia. Gram positive cocci, Gram negative bacilli and Candida albicans were the most common isolates in mild neutropenia compared to Pseudomonas aeruginosa in moderate neutropenia. Urine culture was positive in 18 patients (20.5%) out of 88 with mild neutropenia. Escherichia coli, Pseudomonas aeruginosa and streptococcus viridans were isolated. Urine cultures were negative in all moderate neutropenia cases. Mortality was significantly higher (p<0.0001) in patients with moderate neutropenia (n=8/9, 88.9%) compared to patients with mild neutropenia (n=7/88, 7.9%). No gender predilection on the degree of neutropenia was identified. Infectious foci were identified in 72 patients with mild neutropenia whereas cancer and chemotherapy effect were identified in moderate neutropenia (see Table 2). 3

Table 2: Comparative Analysis of Mild versus Moderate Neutropenia According to Duration and Culture Results Mild Moderate p-values No. of patients 88 9 Age (mean ± SD) 30.67 ± 25.3 yrs 51.33 ± 15.4 yrs 0.0185 Duration of neutropenia (mean ± 2.3 ± 1.17 days 2.67 ± 2.6 days 0.4355 SD) Blood culture positivity 40 (45.5%) 4 (44.4%) 0.9497 Urine culture positivity 18 (20.5%) None Mortality 7 (7.9%) 8 (88.9%) <0.0001 Presence of infective foci 72 (81.8%) 4 (44.5%) 0.0313 Blood culture isolates Gram positive cocci Gram negative bacilli Candida albicans Pseudomonas aeruginosa Febrile neutropenia was seen in 82 patients (84.5%) compared to 15 Neutropenia patients (15.5%) without fever. Those with fever were relatively younger (37.7 ± 25.6 verses 39.82 ± 21.1 years, p=0.7632) and with shorter duration of neutropenic episodes (2.33 ± 1.3 verses 2.53 ± 1.8 days, p=0.6083). Foci of infection were identified in 85.4% of febrile neutropenia, significantly greater than 40% in non-febrile neutropenia (p=0.0009). Blood culture positivity was significantly greater in febrile neutropenia than non-febrile neutropenia (50% verses 20%, p=0.0120). However, mortality was significantly lower in non-febrile than in febrile neutropenia (11% vs. 40%, p=0.0294). In 82 patients (84.5%), neutropenia eventually resolved before being discharged from the hospital (see Table 3). Table 3: Comparison between Febrile and Non-febrile Neutropenia in 97 Neutropenia Cases With Fever Without Fever p-values No. of patients 82 15 Age (mean ± SD) 37.7 ± 25.6 yrs 39.82 ± 21.1 yrs 0.7632 No. of hospital days (mean ± SD) 9.77 ± 7.8 days 24.47 ± 28.3 days 0.0001 Duration of neutropenia 2.33 ± 1.3 days 2.53 ± 1.8 days 0.6083 (mean ± SD) Absolute Neutrophil count 1183.3 ± 243 1020 ± 355 0.1377 (mean ± SD) Focus of Infection present 70 (85.4%) 6 (40%) 0.0009 Blood culture positivity 41 (50%) 3 (20%) 0.0120 Urine culture positivity 14 (17%) 4 (26.7%) 0.4307 Mortality 9 (11%) 6 (40%) 0.0294 Gram negative bacilli Candida albicans Common isolates Gram positive cocci Pseudomonas 4

aeruginosa DISCUSSION Based on the WHO classification, our study showed that neutropenia occurs more commonly in females and that elderly individuals have a higher incidence rate than younger individuals as previously described in the literature 1,2,3,18,19. The high number of infection as a cause of neutropenia is often discovered in the course of an acute infection and the neutropenia is secondary to the infection itself rather than a predisposing factor 4. Several other factors may have contributed to the neutropenic status of our patients such as immunosuppressive drugs and the condition of the immune system 5-11. These have limited the result of our study. Elderly individuals tend to have a more severe degree of neutropenia as shown in our results, with higher complication and mortality rate. Our study showed that elderly individuals have a more severe degree of neutropenia. This is in contrast to studies done in children where high incidence of a more severe degree of neutropenia has been reported 13. The high incidence of fungal isolates from patients presenting with neutropenia have been reported. Our study has shown Candida albicans isolated from a non-febrile patient 14. Furthermore, Gram positive and Gram negative organisms such as Escherichia coli, Pseudomonas aeruginosa, and Streptococcus viridans were common isolates, similar to previous studies 13-17. Fever served as an alarm for the physicians to aggressively investigate and manage the cause of neutropenia. This is why the mortality rate was relatively higher among patients who did not present with fever since physicians were caught unaware of the seriousness of the condition. This is true of the fact that neutropenia in these cases went undetected and discovered only when patients presented with fever, developed a serious infection or was in a life-threatening condition. Patients with neutropenia should be considered initially for risks assessment and initiation of more aggressive management protocols. CONCLUSION Our study suggests that in neutropenia, there is a need to consider a variety of factors such as age, sex, infectious foci, presence of fever and even the duration of neutropenia for the initiation of appropriate management protocols. REFERENCES 1. Kyono W, Coates TD. A practical Approach to Neutrophil Disorders. Pediatr Clin North Am 2002; 49:929-71. 2. Skokowa J, Germeshausen M, Zeidler C, et al. Severe Congenital Neutropenia: Inheritance and Pathophysiology. Curr Opin Hematol 2007; 14:22-8. 3. Durnaa B, Dzierzanowska D. Infection in Neutropenic Cancer Patients - Etiology, Microbiological Diagnostics, Treatment. Wiad Lek 2006; 59:506-11. 4. Vlacha V, Feketea G. The Clinical Significance of Non-malignant Neutropenia in Hospitalized Children. Ann Hematol 2007; 86(12):865-70. 5. Sedky K, Lippmann S. Psychotropic Medications and Leucopenia. Curr Drug Targets 2006; 7:1191-4. 6. Kohli U, Gulati S. Valproate Induced Isolated Neutropenia. Ind J Pediatr 2006; 73:844. 5

7. Scheetz MH, McKoy JM, Parada JP, et al. Systematic Review of Piperacillininduced Neutropenia. Drug Saf 2007; 30:295-306. 8. Pontikoglou C, Liapakis G, Pyrovolaki K, et al. Evidence for down regulation of Erythropoietin Receptor in Bone Marrow Erythroid Cells of Patients with Chronic Idiopathic Neutropenia. Exp Hematol 2006; 34:1312-22. 9. Doulgeraki A, Kotsonis K, Lianou D, et al. An Interesting Case of Primary Autoimmune Neutropenia. Clin Pediatr 2007; 46:266-7. 10. Moores KG. Safe and Effective Outpatient Treatment of Adults with Chemotherapy Induced Neutropenic Fever. Am J Health Syst Pharm 2007; 64: 717-22. 11. Lyman GH. Risks and Consequences of Chemotherapy-induced Neutropenia. Clin Cornerstone 2006; 8(5):S12-8. 12. Watts RG. Neutropenia. In: Lee GR, Forester J, Lukens J, et al, eds. Wintrobe s Clinical Hematology. Vol 1, 10 th ed. Baltimore, Md: Williams & Wilkins; 1999; 1862-88. 13. Arnello LM, Quintana BJA, Barraza CP. Febrile Neutropenia in Children with Cancer in a Medical Center of Santiago, Chile. Rev Chilena Infectol 2007; 24:27-32. 14. Kara IO, Tasova Y, Uguz A, et al. Mucormycosis-associated Fungal Infections in Patients with Haematologic Malignancies. Int J Clin Pract 2007; 16: abstract (Epub ahead of print). 15. Egyed M, Kollar B, Karadi E, et al. Neutropenia and Sepsis in Hematologic Patients. Orv Hetil 2006; 147:2031-3. 16. Figuera Esparza M, Carballo M, Silva M, et al. Microbiological Isolates in Patients with Febrile Neutropenia and Hematological Malignancies. Rev Esp Quimioter 2006; 19:247-51. 17. Kibbler CC, Prentice HG. Pathogen Shift in Febrile Neutropenia. Curr Opin Infect Dis 1999; 12:351-4. 18. Godwin JE. Neutropenia. http://www.emedicine.com/med/topic1640.htm. 2005. Accessed on July 2007. 19. Hsieh MM, Everhart JE, Byrd-Holt DD, et al. Prevalence of Neutropenia in the US Population: Age, Sex, Smoking Status and Ethnic Differences. Ann Intern Med 2007; 146:486-92. 6