Mpox Cases Among Cisgender Women and Pregnant Persons — United States, May 11–November 7, 2022

Weekly / January 6, 2023 / 72(1);9–14

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Lisa P. Oakley, PhD1,*; Kaitlin Hufstetler, MD1,2,*; Jesse O’Shea, MD1; J. Danielle Sharpe, PhD1,3; Cristin McArdle, PhD1,3; Varsha Neelam, MPH1; Nicole M. Roth, MPH1; Emily O. Olsen, PhD1; Maren Wolf, MPH1,3; Leah Zilversmit Pao, PhD1; Jeremy A. W. Gold, MD1; K. Meryl Davis, MD1,2; Dana Perella, MPH4; Shara Epstein, MD4; Maura K. Lash, MPH5; Olivia Samson, MPH5; Jessica Pavlick, DrPH6; Amanda Feldpausch, DVM6; Jennifer Wallace, MD7; Atmaram Nambiar, MD7; Van Ngo, MPH8; Umme-Aiman Halai, MD8; Claudia W. Richardson, MD9; Traci Fowler, DNP10; Burnestine P. Taylor, MD11; Joyce Chou, MSPH12; Lindsey Brandon, MSN13; Rose Devasia, MD14; Erin K. Ricketts, MD3,15; Catherine Stockdale16; Mellisa Roskosky, PhD3,16; Rachel Ostadkar17; Yeng Vang17; Romeo R. Galang, MD1; Kiran Perkins, MD1; Melanie Taylor, MD1; Mary Joung Choi, MD1; Paul J. Weidle, PharmD1; Patrick Dawson, PhD1; Sascha Ellington, PhD1; CDC Mpox Analytics Team (View author affiliations)

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Summary

What is already known about this topic?

Data from the ongoing monkeypox (mpox) outbreak on cases in cisgender women and in pregnancy are limited.

What is added by this report?

Among 769 mpox cases reported among U.S. cisgender women, Black or African American and Hispanic or Latino women were disproportionately affected. Most cisgender women reported recent sexual activity with men. Twenty-three cases among pregnant or recently pregnant persons were reported and all recovered. Four pregnant persons were hospitalized for mpox, and tecovirimat was tolerated with no adverse reactions.

What are the implications for public health practice?

Continued monitoring of mpox risk in cisgender women and during pregnancy is critical to assessing the impacts of mpox on sexual, reproductive, and overall health and to better understand perinatal outcomes.

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Monkeypox (mpox) cases in the 2022 outbreak have primarily occurred among adult gay, bisexual, and other men who have sex with men (MSM); however, other populations have also been affected (1). To date, data on mpox in cisgender women and pregnant persons have been limited. Understanding transmission in these populations is critical for mpox prevention. In addition, among pregnant persons, Monkeypox virus can be transmitted to the fetus during pregnancy or to the neonate through close contact during or after birth (25). Adverse pregnancy outcomes, including spontaneous abortion and stillbirth, have been reported in previous mpox outbreaks (3). During May 11–November 7, 2022, CDC and U.S. jurisdictional health departments identified mpox in 769 cisgender women aged ≥15 years, representing 2.7% of all reported mpox cases. Among cases with available data, 44% occurred in cisgender women who were non-Hispanic Black or African American (Black), 25% who were non-Hispanic White (White), and 23% who were Hispanic or Latino (Hispanic). Among cisgender women with available data, 73% reported sexual activity or close intimate contact as the likely route of exposure, with mpox lesions most frequently reported on the legs, arms, and genitals. Twenty-three mpox cases were reported in persons who were pregnant or recently pregnant§; all identified as cisgender women based on the mpox case report form. Four pregnant persons required hospitalization for mpox. Eleven pregnant persons received tecovirimat, and no adverse reactions were reported. Continued studies on mpox transmission risks in populations less commonly affected during the outbreak, including cisgender women and pregnant persons, are important to assess and understand the impact of mpox on sexual, reproductive, and overall health.

Data on confirmed and probable cases of mpox are electronically reported as part of national case surveillance through a standardized case report form or the National Notifiable Diseases Surveillance System.** Data are collected by health departments and include demographic characteristics, possible exposure routes, and signs and symptoms. CDC analyzed case report data for probable or confirmed†† cases among cisgender women aged ≥15 years and pregnant persons during May 11–November 7, 2022. In addition, CDC identified all persons with mpox reported to CDC through national case surveillance and clinical consultations who were pregnant or recently pregnant regardless of gender identity. Detailed data regarding maternal and neonatal outcomes were obtained through enhanced pregnancy surveillance.§§ Statistical analyses were conducted using SAS statistical software (version 9.4; SAS Institute) and restricted to cases with available data. This activity was reviewed by CDC and was conducted consistent with applicable federal law and CDC policy.¶¶

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Cases Among Cisgender Women

During May 11–November 7, 2022, a total of 769 cases of mpox among cisgender women, including 23 (3%) who were pregnant, were reported by 42 public health jurisdictions (Table 1). The median age was 32 years (IQR = 25–40 years). Among the 717 (93%) cisgender women with information on race and ethnicity, 313 (44%) were Black, 182 (25%) were White, and 167 (23%) were Hispanic. Among 463 (60%) cisgender women with information on recent sexual behaviors, 329 (71%) reported recent sexual activity or close intimate contact,*** including 296 (90%) who had recent sexual contact with a cisgender man and 18 (6%) who had recent sexual contact with a cisgender woman. Among the 18 patients who had recent sexual contact with a woman, 12 also had a recent male sex partner. Of the 73 cisgender women who had complete exposure data, 53 (73%) reported recent sexual or intimate contact as the likely route of exposure. Among the 16 who reported household contact or caregiving as the likely route of exposure, five reported recent sexual or intimate contact. Among the 378 cisgender women with available data on immunocompromising conditions, 35 (9%) reported any known immunocompromising condition other than HIV infection. Information on HIV status was available for 173 cisgender women, 13 (8%) of whom had HIV infection; no cisgender women with HIV infection were pregnant.

Among all cisgender women with mpox and available data, the most frequently reported signs and symptoms were rash (93%), headache (54%), pruritis (57%), malaise (54%), fever (49%), and chills (49%) (Table 2). Among 376 (49%) cisgender women with data on rash location, rash was most frequently reported on the legs (48%), arms (47%), genitals (36%), and trunk (33%); 50 (16%) reported rash in one region, 63 (20%) in two regions, 57 (18%) in three regions, and 140 (45%) in four or more regions. Rash location was similar when comparing cisgender women who reported recent sexual exposure with those who did not.

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Cases in Currently and Recently Pregnant Persons

During May 11–November 7, 2022, 23 cases of mpox were reported during pregnancy (21) or within 3 weeks of pregnancy (two); all pregnant and recently pregnant persons with mpox identified as cisgender women on the mpox case report form††† (Table 1). Among 12 currently or recently pregnant persons with available exposure data, nine reported sexual contact and three reported household contact. Among 10 cases in pregnant persons with information on trimester of infection, three occurred during the first, four during the second, and three during the third trimester (Table 3). Rash was present in all persons. Genital lesions were reported by four currently or recently pregnant persons; none reported genital lesions near the time of delivery.

Eleven (48%) pregnant persons received tecovirimat (administered during all trimesters of pregnancy); no medication-related adverse events were reported. Four pregnant persons were hospitalized related to symptoms from Monkeypox virus infection (pain control and treatment of superimposed cellulitis) and remained pregnant at discharge. No pregnant person required intensive care, intubation, or unplanned delivery. None of the pregnant persons received vaccinia immune globulin intravenous (VIGIV) for treatment.
Of the 21 persons who received an mpox diagnosis during pregnancy, three have reported outcomes, including two full-term deliveries without complications (including no transmission to the infant) and one spontaneous abortion at 11 weeks’ gestation. Two pregnant persons experienced mpox symptoms within 3 days after delivery; their newborns developed lesions within 1 week of their symptom onset. Both newborns received oral tecovirimat within 48 hours of developing lesions and were treated for 10–14 days; one received VIGIV. Both newborns responded to treatment, appeared to be in good health, and were discharged home.

One recently pregnant person who was breastfeeding developed lesions 4 days postpartum, including under the breast; this person’s newborn developed symptoms with lesions on the face and chest 6 days later. Two other cisgender women who were not pregnant or recently pregnant were breastfeeding at the time of mpox diagnosis. One woman’s infant was exposed to a symptomatic household contact; she experienced symptoms 2 weeks after the infant’s diagnosis. The second woman received an mpox diagnosis following an occupational exposure; breast milk samples from this person were tested and were negative for Monkeypox virus DNA by polymerase chain reaction testing.§§§

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Discussion

Monkeypox virus infections in cisgender women during May 11–November 7 constituted <3% of total U.S. cases. Consistent with disparities observed overall during the ongoing mpox epidemic, the proportion of Black and Hispanic women with mpox was higher than the proportion of Black and Hispanic women in the U.S. population (6). This finding is similar to disparities among mpox cases in the United States overall and underscores the continued need for public health efforts to provide education on prevention of mpox and ensure equitable access to mpox vaccination, testing, and treatment.

Sex or close intimate contact within 3 weeks of symptom onset was reported by nearly three quarters of cisgender women with mpox, and genital lesions were frequently reported, suggesting sexual exposure as a likely primary route of transmission. Obstetrician-gynecologists and other providers should consider mpox when examining new genital, oral, or breast lesions. Patient education regarding risks for transmission of Monkeypox virus and other sexually transmitted infections should be provided.

Genital lesions in pregnant persons pose a risk for Monkeypox virus transmission to the fetus during vaginal delivery.¶¶¶ A thorough skin and mucosal (e.g., anal, vaginal, and oral) examination for mpox lesions should be performed in persons with possible mpox near the time of delivery to identify lesions of which they might be unaware. When mpox lesions, including genital lesions, are present, shared decision-making should be considered when discussing route of delivery. Because there might be an increased risk for severe disease in newborns, breastfeeding should be temporarily delayed until criteria for discontinuing isolation have been met (lesions have resolved, the scabs have fallen off, and a fresh layer of intact skin has formed).****

Clinicians caring for cisgender women and pregnant persons should become familiar with clinical considerations for the prevention, diagnosis, and treatment of mpox†††† and should provide pre- and postexposure prophylaxis if indicated. Vaccination with JYNNEOS should be provided to eligible persons, including those who are pregnant or breastfeeding, and providers should discuss vaccination risks and benefits.§§§§

The findings in this report are subject to at least three limitations. First, data for some variables such as exposure risk and HIV status were frequently missing (≤92%). Thus, these data might not represent the characteristics of the overall sample. Second, the small sample size of currently and recently pregnant persons with mpox might limit the generalizability of outcomes. Finally, additional time is needed for pregnancy completion to describe outcomes among all cases of mpox during pregnancy.

Cases of mpox have occurred primarily among adult gay, bisexual, and other MSM during the current outbreak; however, any person, including cisgender women, can also acquire infection. Public health efforts should include more emphasis on cisgender women who might be at increased risk for exposure. In addition, although most reported cases of mpox in pregnant persons have been managed in the outpatient setting, some persons might require hospitalization, and there is a risk for perinatal transmission. To mitigate this risk, pregnant, recently pregnant, and breastfeeding persons should be offered prophylaxis or treatment if indicated. Continued collection of information is critical to evaluating the risk for transmission, informing infection prevention and control, and assessing the impact of mpox on the sexual, reproductive, and overall health of cisgender women. In addition, collection of longitudinal data among pregnant persons and their infants is critical to understanding the effects of mpox on maternal and neonatal outcomes. CDC, in collaboration with health departments, will continue to follow cases in pregnant and recently pregnant persons and provide updates as data become available.

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Acknowledgments

Mpox response teams from state and local health departments; hospital and clinical providers involved in CDC clinical consultations; Suzanne Newton, Ruth Stefanos, CDC; Thandiwe Bobb, Georgia Department of Public Health; Kay Hooshmand, Chase Israel, Claire Park, Jasmine Sharma, Los Angeles County Department of Public Health; mpox case investigation and response staff members at Acute Communicable Disease Control Program and Community Field Services Division, Los Angeles County Department of Public Health; Marcie Babcock, Victor Cruz, Minnesota Department of Health; Jennifer MacFarquhar, CDC Career Epidemiology Field Officer, North Carolina Department of Health and Human Services; Karen Alroy, Ellen Lee, New York City Department of Health and Mental Hygiene; Lisa McHugh, W. Gina Pang, Nottasorn Plipate, Kumar Nalluswami, Arlene Seid, Pennsylvania Department of Health; Lenore Asbel, Aasta Mehta, Ayomide Sokale, Philadelphia Department of Public Health; Division of Disease Control Response Team, Philadelphia Department of Public Health; Hospital Obstetrics/Gynecology and Infectious Disease Partners, Philadelphia, Pennsylvania; Public Health – Seattle & King County Communicable Disease Investigations Team; Liz Harris, Robertson Nash, Pamela Talley, Tennessee Department of Health; Nicholas Hysmith, LeBonheur Children’s Hospital; Sandra Castejon-Ramirez, St. Jude Children’s Research Hospital, LeBonheur Children’s Hospital.

CDC Mpox Analytics Team

Cori Dennison, CDC; Ian Hennessee, CDC; Aspen Riser, CDC; LaTweika Salmon-Trejo, CDC; Gail Scogin, CDC; Emily Sims, CDC; Penelope Strid, CDC; Raquel Velazquez-Kronen, CDC; Claire Xu, CDC; Carla Zelaya, CDC.

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Corresponding author: Sascha Ellington, sellington@cdc.gov.

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1CDC Mpox Emergency Response Team; 2CDC Foundation, Atlanta, Georgia; 3Epidemic Intelligence Service, CDC; 4Philadelphia Department of Public Health, Philadelphia, Pennsylvania; 5New York City Department of Health and Mental Hygiene, New York, New York; 6Georgia Department of Public Health; 7Pennsylvania Department of Health; 8Los Angeles County Department of Public Health, Los Angeles, California; 9Detroit Health Department, Detroit, Michigan; 10Michigan Department of Health & Human Services; 11Alabama Department of Public Health; 12Missouri Department of Health and Senior Services; 13Shelby County Health Department, Memphis, Tennessee; 14Tennessee Department of Health; 15North Carolina Department of Health and Human Services; 16Communicable Disease, Epidemiology and Immunizations, Public Health – Seattle & King County, Seattle, Washington; 17Minnesota Department of Health.

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All authors have completed and submitted the International Committee of Medical Journal Editors form for disclosure of potential conflicts of interest. No potential conflicts of interest were disclosed.

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* These authors contributed equally to this report.

https://www.cdc.gov/poxvirus/monkeypox/response/2022/demographics.html (Accessed November 7, 2022).

§ Recently pregnant persons had confirmed or probable Monkeypox virus infection within 21 days of delivery.

https://www.cdc.gov/poxvirus/monkeypox/health-departments/case-reporting.html

** https://www.cdc.gov/nndss/index.html

†† https://www.cdc.gov/poxvirus/monkeypox/clinicians/case-definition.html

§§ Enhanced pregnancy surveillance data were collected through direct communication with jurisdictions, under an Assurance of Confidentiality, leveraging existing mother-baby linked surveillance. https://www.cdc.gov/ncbddd/set-net/index.html

¶¶ 45 C.F.R. part 46.102(l)(2), 21 C.F.R. part 56; 42 U.S.C. Sect. 241(d); 5 U.S.C. Sect. 552a; 44 U.S.C. Sect. 3501 et seq.

*** Defined as any sex or close intimate contact during the 3 weeks before symptom onset.

††† CDC recognizes that not all pregnant persons are cisgender women. However, in the study, all cases of mpox in pregnant persons, recently pregnant persons, and breastfeeding persons occurred in persons who identified as cisgender women based on the mpox case report form.

§§§ This breastfeeding mother was a health care worker who cared for a symptomatic patient. She later developed atypical features of mpox.

¶¶¶ https://www.cdc.gov/poxvirus/monkeypox/about/science-behind-transmission.html

**** https://www.cdc.gov/poxvirus/monkeypox/clinicians/pregnancy.html#contact-breastfeeding

†††† https://www.cdc.gov/poxvirus/monkeypox/clinicians/pregnancy.html

§§§§ https://www.cdc.gov/poxvirus/monkeypox/interim-considerations/jynneos-vaccine.html

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References

  1. Blackburn D, Roth NM, Gold JA, et al. Epidemiologic and clinical features of mpox in transgender and gender-diverse adults—United States, May–November 2022. MMWR Morb Mortal Wkly Rep 2022;71:1605–9. https://doi.org/10.15585/mmwr.mm715152a1
  2. Meaney-Delman DM, Galang RR, Petersen BW, Jamieson DJ. A primer on Monkeypox virus for obstetrician-gynecologists: diagnosis, prevention, and treatment. Obstet Gynecol 2022;140:391–7. https://doi.org/10.1097/AOG.0000000000004909 PMID:36356237
  3. D’Antonio F, Pagani G, Buca D, Khalil A. Monkeypox infection in pregnancy: a systematic review and metaanalysis. Am J Obstet Gynecol MFM 2023;5:100747. https://doi.org/10.1016/j.ajogmf.2022.100747 PMID:36096413
  4. Thornhill JP, Palich R, Ghosn J, et al.; Share-Net writing group. Human Monkeypox virus infection in women and non-binary individuals during the 2022 outbreaks: a global case series. Lancet 2022;400:1953–65. https://doi.org/10.1016/S0140-6736(22)02187-0 PMID:36403584
  5. Ramnarayan P, Mitting R, Whittaker E, et al.; National Health Service England High Consequence Infectious Diseases (Airborne) Network. Neonatal monkeypox virus infection. N Engl J Med 2022;387:1618–20. https://doi.org/10.1056/NEJMc2210828 PMID:36223535
  6. Philpott D, Hughes CM, Alroy KA, et al.; CDC Multinational Monkeypox Response Team. Epidemiologic and clinical characteristics of monkeypox cases—United States, May 17–July 22, 2022. MMWR Morb Mortal Wkly Rep 2022;71:1018–22. https://doi.org/10.15585/mmwr.mm7132e3 PMID:35951487

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TABLE 1. Characteristics of cisgender women with mpox, by current or recent* pregnancy status — United States, May 11–November 7, 2022Return to your place in the text
Characteristic (no. with available information) No. (%)§ of cisgender women with mpox
All Not currently or recently pregnant Currently or recently pregnant
Total (769) 769 (100.0) 746 (97.0) 23 (3.0)
Gender identity (769)
Cisgender woman 769 (100.0) 746 (100.0) 23 (100.0)
Age (765)
Median, yrs (IQR)(range) 32 (25–40) (15–89) 32 (25–40) (15–89) 28.5 (23–32) (20–35)
Missing 4 4 0
Race and ethnicity (717) 717 (100.0) 696 (93.3) 21 (91.3)
American Indian or Alaska Native, non-Hispanic 4 (0.6) 4 (0.6) 0 (—)
Asian, non-Hispanic 18 (2.5) 18 (2.6) 0 (—)
Black or African American, non-Hispanic 313 (43.7) 298 (42.8) 15 (71.4)
Hispanic or Latino 167 (23.3) 165 (23.7) 2 (9.5)
Native Hawaiian or other Pacific Islander, non-Hispanic 1 (0.1) 1 (0.1) 0 (—)
White, non-Hispanic 182 (25.4) 179 (25.7) 3 (14.3)
Multiple races, non-Hispanic 10 (1.4) 10 (1.4) 0 (—)
Other race, non-Hispanic 22 (3.1) 21 (3.0) 1 (4.8)
Missing 52 50 2
Recent sexual partners (463)** 463 (100.0) 446 (60.0) 17 (73.9)
Had a recent sexual partner 329 (71.1) 317 (71.1) 12 (70.6)
Gender of recent sexual partners††
Cisgender man 296 (90.0) 284 (89.6) 12 (100.0)
Cisgender woman 18 (5.5) 18 (5.7) 0 (—)
Transgender man 2 (0.6) 2 (0.6) 0 (—)
Transgender woman 0 (—) 0 (—) 0 (—)
Other gender identity 2 (0.6) 2 (0.6) 0 (—)
Exposure (73)§§ 73 (100.0) 61 (8.2) 12 (52.2)
Sexual or intimate 53 (72.6) 44 (72.1) 9 (75.0)
Household or caregiving 16 (21.9) 13 (21.3) 3 (25.0)
Shared food, utensils, or dishes 12 (18.2) 12 (19.7) 0 (—)
Shared towels or bedding 16 (24.2) 16 (26.2) 0 (—)
Shared transportation 10 (15.2) 10 (16.4) 0 (—)
Face-to-face 14 (21.2) 14 (23.0) 0 (—)
Shared bathrooms 15 (22.7) 15 (24.6) 0 (—)
Other 16 (24.2) 16 (26.2) 0 (—)
Health conditions
Immunocompromised (excluding HIV) (378)¶¶ 35 (9.3) 34 (9.3)*** 1 (7.1)†††
HIV infection (173) 13 (7.5) 13 (8.1)§§§ 0 (—)¶¶¶

Abbreviation: mpox = monkeypox.
* Recently pregnant persons had confirmed or probable mpox infection within 21 days of delivery.
Data as of November 9, 2022.
§ Percentages calculated using nonmissing data.
Information on pregnant and recently pregnant persons was gathered by the national surveillance form, clinical consultation, and enhanced pregnancy surveillance.
** Sexual partner during the 3 weeks before symptom onset.
†† Percentage of those who had a sexual partner during the 3 weeks before symptom onset.
§§ Exposures are not mutually exclusive.
¶¶ Immunocompromising conditions include diseases (e.g., diabetes, lupus, organ transplants, stem cell transplants, and cancer) or certain medicines (e.g., chemotherapy, biologic therapies, and steroids).
*** Percentage among the 364 cisgender women who are not currently or recently pregnant with data available on any known immunocompromising conditions.
††† Percentage among the 14 pregnant or recently pregnant persons with data available on any known immunocompromising conditions.
§§§ Percentage among the 161 cisgender women who are not currently or recently pregnant with data available on HIV status.
¶¶¶ Percentage among the 12 pregnant or recently pregnant persons with data available on HIV status.

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TABLE 2. Signs and symptoms and rash sites among all cisgender women with mpox (N = 769) — United States, May 11–November 7, 2022*Return to your place in the text
Characteristic Presence or absence of signs or symptoms, no. (%) No. missing
(% of total sample)
Present Absent Unknown
Sign or symptom
Rash 376 (92.6) 17 (4.2) 13 (3.2) 363 (47.2)
Headache 182 (54.3) 122 (36.4) 31 (9.3) 434 (56.4)
Malaise 176 (53.5) 115 (35.0) 38 (11.6) 440 (57.2)
Fever 165 (48.5) 139 (40.9) 36 (10.6) 429 (55.8)
Chills 162 (49.2) 135 (41.0) 32 (9.7) 440 (57.2)
Pruritis 164 (56.8) 91 (31.5) 34 (11.8) 480 (62.4)
Myalgia 142 (45.1) 142 (45.1) 31 (9.8) 454 (59.0)
Enlarged lymph nodes 137 (41.8) 153 (46.7) 38 (11.6) 441 (57.3)
Vomiting or nausea 63 (24.3) 161 (62.2) 35 (13.5) 510 (66.3)
Abdominal pain 57 (19.2) 198 (66.7) 42 (14.1) 472 (61.4)
Rectal pain 39 (12.8) 229 (74.8) 38 (12.4) 463 (60.2)
Tenesmus 22 (8.5) 199 (76.8) 38 (14.7) 510 (66.3)
Conjunctivitis 14 (5.7) 199 (80.2) 35 (14.1) 521 (67.8)
Pus or blood in stools 12 (4.6) 210 (80.5) 39 (14.9) 508 (66.1)
Rectal bleeding 11 (3.7) 246 (82.8) 40 (13.5) 472 (61.4)
Proctitis 8 (3.3) 185 (76.5) 49 (20.3) 527 (68.5)
Rash site§
Legs 182 (48.4) NA NA NA
Arms 178 (47.3)
Trunk 125 (33.2)
Genitals 137 (36.4)
Face 116 (30.9)
Palms 81 (21.5)
Head 79 (21.0)
Hand 73 (19.4)
Neck 54 (14.4)
Mouth 57 (15.2)
Perianal 53 (14.1)
Soles 44 (11.7)
Other 100 (26.6)

Abbreviation: NA = not applicable.
* Data as of November 9, 2022.
Percentages calculated using nonmissing data.
§ Percentages among the 376 cisgender women who reported experiencing rash.

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TABLE 3. Characteristics of currently and recently pregnant persons* with mpox (N = 23) — United States, May 11–November 7, 2022Return to your place in the text
Characteristic No. (%)
Currently pregnant 21 (91.3)
Recently pregnant 2 (8.7)
Pregnancy trimester when Monkeypox virus infection occurred (10)
First 3 (30.0)
Second 4 (40.0)
Third 3 (30.0)
Missing 11
Sign or symptom§
Fever 6 (26.1)
Rash 23 (100.0)
Genital or breast lesions 4 (17.4)
Myalgia 2 (8.7)
Pruritis 6 (26.1)
Lymphadenopathy 3 (13.0)
Disease severity
Hospitalized
Yes 4 (17.4)
No 19 (82.6)
Admitted to ICU 0 (—)
Mpox-directed therapy
Tecovirimat (oral or IV) 11 (47.8)
VIGIV 0 (—)
Postexposure prophylaxis
Received JYNNEOS 0 (—)

Abbreviations: ICU = intensive care unit; IV = intravenous; mpox = monkeypox; VIGIV= vaccinia immune globulin intravenous.
* Recently pregnant persons had confirmed or probable Monkeypox virus infection within 21 days of delivery.
Percentages calculated among nonmissing values.
§ Signs and symptoms are not mutually exclusive.
Two women who received tecovirimat also received other treatments (e.g., acyclovir or antibiotics).

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Suggested citation for this article: Oakley LP, Hufstetler K, O’Shea J, et al. Mpox Cases Among Cisgender Women and Pregnant Persons — United States, May 11–November 7, 2022. MMWR Morb Mortal Wkly Rep 2023;72:9–14. DOI: http://dx.doi.org/10.15585/mmwr.mm7201a2.

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