Mumps (mumps parotitis)

Virology, transmission, and epidemiology

• Pathogen Paramyxovirus, negative-sense single-stranded RNA, enveloped, two surface proteins: hemagglutinin-neuraminidase (HN - cell receptor sialic acid binding) and fusion protein (F - membrane fusion and viral entry), 12 identified genotypes (A through N), genotypes C, D, G, H, and J currently most prevalent in North America, vaccines based on the Jeryl Lynn strain (genotype A) provide effective cross-protection against the majority of circulating genotypes despite genetic divergences
• Transmission: respiratory droplets (coughing + sneezing + talking) + direct contact with infected saliva (kissing + sharing utensils + sharing bottles) + the virus is present in saliva 7 days before the onset of parotitis up to 9 days after + maximal contagiousness period in the 2 days before and 5 days after the onset of symptoms
• Incubation period: 16 to 18 days (range: 12 to 25 days) + one of the longest incubations among common viral infections
• Pathogenesis: primary replication in the respiratory epithelium + viremia → dissemination to salivary glands (parotid ++), testes, ovaries, pancreas, meninges, inner ear + glandular acinar cell affection → inflammation + edema + local cell necrosis
• Epidemiology in Quebec: fewer than 100 cases reported annually since the 1990s + sporadic epidemics associated with university campuses + summer camps + religious communities refusing vaccination + importations during international travel + young adults born between 1970 and 1985 (having received only one dose of vaccine in childhood) represent a risk group during outbreaks

Clinical presentation

Complications

Biological diagnosis

• RT-PCR (reverse transcription polymerase chain reaction) on oral or urine sample: reference method + saliva or oral swab collection + to be performed within 9 days of the onset of parotitis (maximum sensitivity within the first 3 days) + allows for direct detection of viral genome + typing of the epidemic genotype for epidemiological surveillance + method recommended by the Institut national de santé publique du Québec (INSPQ) for case confirmation in an epidemic context
• Serology (IgM and IgG anti-mumps virus): IgM anti-mumps → present from the 3rd-5th day after symptom onset + persist for 2-3 months + indicate recent infection + can be falsely negative in the early days and in vaccinated individuals (attenuated IgM response in case of revaccination) + IgG → present 1-2 weeks after onset + persist for life (natural or vaccine-induced immunity) + seroconversion (rise in IgG titer between two samples 14 days apart) confirms acute infection in cases of negative IgM
• Additional biological assessment based on complications: serum lipase and amylase (pancreatitis) + CBC (leukopenia + relative lymphocytosis often seen in viral infections) + CSF if meningitis suspected (lymphocytic pleocytosis + mumps PCR on CSF) + audiometry if hearing loss
• Salivary amylase (S isoenzyme): Mumps (viral + bacterial + salivary calculi) can suggest the diagnosis but is not specific. Elevated total amylase in mumps does not necessarily indicate pancreatitis (pancreatic amylase P + salivary amylase S both contribute to total amylase).

Prevention — MMR vaccination and Quebec context

• MMR Vaccine (Measles-Mumps-Rubella): trivalent live attenuated vaccine containing vaccine strains Edmonston (measles) + RA27/3 (rubella) + Jeryl Lynn or RIT 4385 (mumps) + administered in two doses in the Quebec Immunization Program (QIP): 1st dose at 12 months + 2nd dose at 18 months (or catch-up upon entering kindergarten) + two doses offer protective efficacy against mumps of 88 %(95% CI %: 67–95 %) — slightly lower than that against measles (97 % ) and rubella (94 % )
• Vaccine catch-up for adults: Anyone born after 1969 in Quebec must have received two documented doses of the MMR vaccine. Adults without proof of vaccination or born before 1970 (assumed to have natural immunity) may receive a catch-up dose if there is a risk of exposure. The RAMQ reimburses the MMR vaccine for adult catch-up according to PQI criteria.
• Third dose in an epidemic context: during documented outbreaks in closed communities (university campuses + military facilities + summer camps) → a third dose of MMR may be recommended by the Public Health Department for people at high risk of exposure + effectiveness of a 3rd dose estimated at 88 % for the prevention of mumps during direct exposure
• Contraindications to MMR vaccine: Pregnancy (live attenuated vaccine + avoid pregnancy for 4 weeks after vaccination) + severe immunosuppression (chemotherapy + high-dose corticosteroids + advanced stage AIDS) + history of anaphylactic reaction to vaccine components (hydrolyzed porcine gelatin + neomycin) + egg allergy is not an absolute contraindication in current practice (modern MMR vaccine contains minimal traces of egg protein + administrable in a monitored medical setting)
• Control measures during a case: Mandatory reporting (MADO) to the Regional Public Health Department (DRSP) within 24–48 hours + exclusion from school or community for 5 days after symptom onset + identification and vaccination of unvaccinated contacts (vaccination within 72 hours can reduce risk in exposed contacts)

Consult at Clinique Omicron

Clinique Omicron's physicians and nurse practitioners (NPs) diagnose and manage mumps and its complications, prescribe mumps RT-PCR and serology, perform mandatory public health reporting, assess vaccination status and administer catch-up MMR vaccine to unvaccinated adults, and refer to ENT for auditory symptoms or to urology for severe orchitis. Consultations are available at several service points in Quebec and via telemedicine. To book an appointment, visit cliniqueomicron.ca.

The content of this page is for informational purposes only and does not replace medical advice. Mumps is a reportable disease in Quebec — any confirmed or suspected case must be reported to the Regional Public Health Directorate. Two-dose MMR vaccination remains the most effective way to prevent mumps and its complications.