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Volume 30, Number 7—July 2024
Dispatch

Rocky Mountain Spotted Fever Mimicking Multisystem Inflammatory Syndrome in Hospitalized Children, Sonora, Mexico

Author affiliations: University of Sonora, Hermosillo, Mexico (G. Álvarez-Hernández, C.N. Rivera-Rosas, J.R.T. Calleja-López); Centers for Disease Control and Prevention, Atlanta, Georgia, USA (D.W. McCormick, C.D. Paddock); Sonora Children’s Hospital, Hermosillo (J.B. Álvarez-Meza); Centro Nacional de Programas Preventivos y Control de Enfermedades, Mexico City, Mexico (F. Correa-Morales)

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Abstract

We describe 5 children who had Rocky Mountain spotted fever (RMSF) and manifested clinical symptoms similar to multisystem inflammatory syndrome in Sonora, Mexico, where RMSF is hyperendemic. Physicians should consider RMSF in differential diagnoses of hospitalized patients with multisystem inflammatory syndrome to prevent illness and death caused by rickettsial disease.

Rocky Mountain spotted fever (RMSF), a tickborne disease caused by Rickettsia rickettsii, is the leading cause of death from rickettsial infections in the Western Hemisphere (1). The disease can progress rapidly to death or severe illness in persons who do not receive appropriate antimicrobial drug therapy within the first 5 days after illness onset (13).

Hyperendemic RMSF levels are present in several communities in the southwestern United States and multiple states across northern Mexico (4). Case-fatality rates in northern Mexico are 27%–33% (5,6). A total of 2,176 RMSF cases were identified in Mexico during 2015–2023, of which 933 (42.9%) patients were children and adolescents 1 month–19 years of age (7). Sonora, in northwestern Mexico, has the greatest RMSF burden within the country; 222 pediatric cases were identified during 2015–2022, comprising ≈50% of the state’s total RMSF incidence during that period (6).

During March 2020–December 31, 2022, a total of 16,207 pediatric cases of COVID-19 occurred in Sonora, of which 434 (2.7%) case-patients were hospitalized and 36 died (case-fatality rate 0.22%) (8). However, national- or state-level data are not available for cases of multisystem inflammatory syndrome in children (MIS-C). The early signs and symptoms of RMSF are nonspecific and include fever, headache, rash, nausea, vomiting, arthralgia, and myalgia. Early manifestations of RMSF often resemble other common pediatric febrile illnesses, such as Kawasaki disease and toxic shock syndrome (13). As RMSF progresses, abdominal pain, extremity edema, dyspnea, tachycardia, hypotension, organ edema, hemorrhages, septic shock, distal necrosis of the extremities, and death can occur (3,9). The clinical profile of MIS-C (10,11) overlaps with that of severe rickettsioses, particularly during the later stages of RMSF infections, and this clinical similarity might lead to critical gaps in prompt diagnosis and treatment of both diseases in endemic regions. We describe 5 pediatric patients with RMSF admitted to a hospital in Sonora who were initially suspected of having MIS-C.

The Study

We identified patients after reviewing 8,432 inpatient admissions at the Sonora Children’s Hospital in Hermosillo, Mexico, during September 30, 2020–December 31, 2022. During the study period, RMSF was diagnosed in 61 patients, COVID-19 in 27 patients, and MIS-C in 13/27 (48%) patients who had COVID-19 (12). We retrieved sociodemographic and clinical characteristics from medical charts. The study was approved by the Sonora Children’s Hospital Institutional Review Board.

We used the World Health Organization case definition to identify patients with MIS-C (13); we defined evidence of COVID-19 as detectable SARS-CoV-2 antibodies in serum samples or a positive antigen test from a nasopharyngeal swab sample. We defined an RMSF case as a patient who had >2 acute clinical manifestations within 7 days, such as fever, headache, malaise, rash, diarrhea, vomiting, and a history of tick exposure, along with a single positive Rickettsia confirmatory test. Confirmatory tests included detection of R. rickettsii or Rickettsia spp. DNA in whole-blood specimens by using quantitative PCR (qPCR) or detection of R. rickettsia–specific IgG at a titer of >1:256 in a single serum specimen by using an indirect immunofluorescence assay.

We identified 5 patients with RMSF who also met World Health Organization criteria for MIS-C. The median patient age was 8 (range 6–17) years; 4 were male and 1 female (Table 1). The median duration from illness onset to hospital admission was 10 (range 4–10) days. All patients had a fever and rash; other common symptoms were abdominal pain in 3 (60%) patients and edema of the hands and feet in 3 (60%) patients. The rash preceded hospital admission in 4 (80%) patients. All patients reported a history of tick exposure and received corticosteroids; 3 received intravenous immunoglobulin for treatment of suspected MIS-C.

R. rickettsii infection was confirmed by IFA for 2 patients whose blood samples were drawn on the 6th and 13th days after onset of symptoms. Two patients were positive for R. rickettsii by qPCR, and qPCR detected Rickettsia spp. in 1 case. Although all patients received their first medical consultation within 1–3 days after onset of symptoms, a delay in clinical suspicion of RMSF beyond day 5 was found in 4 (80%) cases; the median delay in prescribing specific antimicrobial drugs for RMSF was 10 (range 3–13) days after symptom onset (Table 2). Doxycycline treatment was belatedly initiated in all 5 patients, in 4 at the time of hospital admission and in 1 patient 3 days after hospitalization.

Laboratory test abnormalities seen in the 5 patients included thrombocytopenia; elevated inflammatory markers such as C-reactive protein, procalcitonin, D-dimer, ferritin, and aminotransferases; and leukocytosis (Table 1). Four patients were admitted to the hospital’s intensive care unit and required vasopressor support. Echocardiography was performed for 3 patients: 1 patient had no abnormal findings, 1 patient had trace pericardial effusion, and 1 patient had a 0.5 cm pericardial effusion and tricuspid regurgitation. The median duration of hospitalization was 13 (range 3–15) days. No patients died, and severe sequelae were not reported.

Conclusions

RMSF and MIS-C share clinical and laboratory test abnormalities and distinguishing between those 2 conditions can be challenging for clinicians in endemic regions. We describe 5 children who had clinical and laboratory evidence of both RMSF and MIS-C. Those patients improved with doxycycline treatment, highlighting the importance of timely recognition and treatment of RMSF, even when clinicians suspect SARS-CoV-2 infections. Because those infections can co-exist, a high degree of clinical suspicion is necessary. A history of tick exposure should prompt clinicians to consider RMSF, although tick bites are recognized in <50% of RMSF cases.

Clinical suspicion of MIS-C should not preclude consideration of RMSF and other rickettsial diseases (12,13). Fever, rash, gastrointestinal manifestations, and abdominal pain are among the most frequent clinical features in hospitalized children with MIS-C (10) or RMSF (2,3,9). Although ≈90% of patients with MIS-C or RMSF manifest fever, a rash is present in up to 90% of RMSF patients (6), compared with ≈50% of children with MIS-C (10,14). Patients with RMSF and MIS-C have similar laboratory test abnormalities that include thrombocytopenia, hyponatremia, and elevated inflammatory markers (i.e., procalcitonin and C-reactive protein) (6,9,10,14), probably because both diseases are characterized by a generalized inflammatory response, endothelial damage, and increased vascular permeability (1,10).

Doxycycline is the recommended antimicrobial drug treatment for all patients who have suspected RMSF and should be empirically initiated to reduce fatal outcomes and severe sequelae (1,3,9), particularly in vulnerable children living with social disadvantages (1,14). Physicians and other health personnel practicing in RMSF-endemic areas should systematically consider RMSF in the differential diagnosis of hospitalized patients who have MIS-C to reduce delays in therapy and prevent death and severe sequelae caused by this rickettsial disease.

Dr. Álvarez-Hernández is a professor in the Department of Medicine and Health Sciences at the Universidad de Sonora, Mexico. His primary research interests are focused on epidemiology of infectious diseases, particularly tickborne diseases, as well as public health policies.

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References

  1. Biggs  HM, Behravesh  CB, Bradley  KK, Dahlgren  FS, Drexler  NA, Dumler  JS, et al. Diagnosis and management of tickborne rickettsial diseases: Rocky Mountain spotted fever and other spotted fever group rickettsioses, ehrlichioses, and anaplasmosis—United States. MMWR Recomm Rep. 2016;65:144.
  2. Kirkland  KB, Wilkinson  WE, Sexton  DJ. Therapeutic delay and mortality in cases of Rocky Mountain spotted fever. Clin Infect Dis. 1995;20:111821.
  3. Buckingham  SC, Marshall  GS, Schutze  GE, Woods  CR, Jackson  MA, Patterson  LER, et al. Clinical and laboratory features, hospital course, and outcome of Rocky Mountain spotted fever in children. J Pediatr. 2007;150:1804.e1.
  4. Foley  J, Álvarez-Hernández  G, Backus  LH, Kjemtrup  A, Lopéz-Pérez  AM, Paddock  CD, et al. The emergence of Rocky Mountain spotted fever in the southwestern United States and northern Mexico requires a binational One Health approach. J Am Vet Med Assoc. 2024;262:698704.
  5. Zazueta  OE, Armstrong  PA, Márquez-Elguea  A, Hernández Milán  NS, Peterson  AE, Ovalle-Marroquín  DF, et al. Rocky Mountain spotted fever in a large metropolitan center, Mexico–United States border, 2009–2019. Emerg Infect Dis. 2021;27:156776.
  6. Álvarez-López  DI, Ochoa-Mora  E, Nichols Heitman  K, Binder  AM, Álvarez-Hernández  G, Armstrong  PA. Epidemiology and clinical features of Rocky Mountain spotted fever from enhanced surveillance, Sonora, Mexico: 2015–2018. Am J Trop Med Hyg. 2021;104:1907.
  7. Government of Mexico. Ministry of Health, General Director of Epidemiology. Morbidity yearbooks 1984–2022 [in Spanish] [cited 2023 Nov 13]. https://www.gob.mx/salud/acciones-y-programas/anuarios-de-morbilidad-1984-a-2022
  8. Government of Mexico, National Council of Humanities, Science and Technology. COVID-19 dashboard Mexico [in Spanish] [cited 2023 Nov 13]. https://datos.covid-19.conacyt.mx
  9. Alvarez-Hernandez  G, Murillo-Benitez  C, Candia-Plata  MC, Moro  M. Clinical profile and predictors of fatal Rocky Mountain spotted fever in children from Sonora, Mexico. Pediatr Infect Dis J. 2015;34:12530.
  10. Kundu  A, Maji  S, Kumar  S, Bhattacharya  S, Chakraborty  P, Sarkar  J. Clinical aspects and presumed etiology of multisystem inflammatory syndrome in children (MIS-C): a review. Clin Epidemiol Glob Health. 2022;14:100966.
  11. Jiang  L, Tang  K, Irfan  O, Li  X, Zhang  E, Bhutta  Z. Epidemiology, clinical features, and outcomes of multisystem inflammatory syndrome in children (MIS-C) and adolescents—a live systematic review and meta-analysis. Curr Pediatr Rep. 2022;10:1930.
  12. Government of Mexico. Ministry of Health, General Director of Health Information. SINBA. National System of Basic Health Information [in Spanish] [cited 2023 Nov 13]. https://sinba.salud.gob.mx
  13. World Health Organization. Multisystem inflammatory syndrome in children and adolescents with COVID-19. Scientific brief, May 15, 2020 [cited 2024 May 4]. https://www.who.int/publications/i/item/multisystem-inflammatory-syndrome-in-children-and-adolescents-with-covid-19
  14. Álvarez-Hernández  G, Roldán  JFG, Milan  NSH, Lash  RR, Behravesh  CB, Paddock  CD. Rocky Mountain spotted fever in Mexico: past, present, and future. Lancet Infect Dis. 2017;17:e18996.

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Cite This Article

DOI: 10.3201/eid3007.240033

Original Publication Date: June 11, 2024

Table of Contents – Volume 30, Number 7—July 2024

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Gerardo Álvarez-Hernández, University of Sonora, Blvd Luis D. Colosio SN, col. Centro, Hermosillo, CP 83000, Mexico

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Page created: June 06, 2024
Page updated: June 22, 2024
Page reviewed: June 22, 2024
The conclusions, findings, and opinions expressed by authors contributing to this journal do not necessarily reflect the official position of the U.S. Department of Health and Human Services, the Public Health Service, the Centers for Disease Control and Prevention, or the authors' affiliated institutions. Use of trade names is for identification only and does not imply endorsement by any of the groups named above.
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