key: cord-0765201-kbgqzq6v
authors: Ogawa, Eisuke; Goto, Hirohisa; Ushimaru, Hiroyasu; Matsuo, Akemi; Takeda, Satoshi; Nishimura, Ryohei; Hondo, Takaaki; Takahashi, Takashi
title: Vaginal delivery after improvement in COVID-19 by monoclonal antibody treatment: A case report and literature review
date: 2022-03-07
journal: J Infect Chemother
DOI: 10.1016/j.jiac.2022.02.023
sha: e47e1910ddd8e042e81209ce598a1046ab0bb95a
doc_id: 765201
cord_uid: kbgqzq6v

As the COVID-19 pandemic persists, pregnant women have been increasingly affected worldwide. Women during the last trimester of pregnancy are susceptible to severe COVID-19, and there are many challenges towards its treatment. Monoclonal antibody treatment (MAT) is approved for COVID-19 patients to reduce disease severity. However, there are few reports on the MAT in perinatal women. Herein, we report a 39-year-old pregnant female (36 weeks and 6 days of gestation) with improvement in COVID-19 pneumonia after treatment with casiribimab/imdevimab, resulting in successful vaginal delivery (a 2.868 kg male newborn), along with a literature review. Early diagnosis and treatment of pregnant women with COVID-19 are important. Infectious diseases doctors and/or obstetricians should be aware of the MAT option administered to perinatal COVID-19 women to reduce disease severity.

COVID-19 is an infectious disease caused by SARS-CoV-2 and is prevalent worldwide.

The infection rate and risk of hospitalization for COVID- 19 have been reported to increase during pregnancy, and there is a strong concern about the severity of the disease among this population [1] [2] [3] . Pregnant women with COVID-19 have a 3 to 4-folds high risk of being severely ill or hospitalized compared to non-pregnant COVID-19 patients [1, 4, 5] .

Additionally, the risk of death was reported to be about 13-times higher in gravid patients [1] .

Drugs available during both pregnancy and lactation, as well as monoclonal antibody treatment (MAT), may be beneficial in obstetric/perinatal situations. MATs are useful particularly for managing patients with rheumatoid arthritis and inflammatory bowel diseases;

tumor necrosis factor- (TNF-) inhibitors are considered safe to administer based on epidemiological studies and clinical experiences [6] [7] [8] [9] . Casirivimab and imdevimab (C&I, Ronapreve™) combination treatment was approved to attenuate the severe progression of COVID-19 under emergency use permission from the Ministry of Health, Labour and Welfare during the Japanese 5th epidemic in 2021. C&I is a co-package of two neutralizing immunoglobulin gamma 1 human monoclonal antibodies against the Spike protein, especially the receptor-binding domain. However, there are few reports regarding the MAT of perinatal COVID-19 women. We herein report a 39-year-old pregnant woman (36 weeks and 6 days of J o u r n a l P r e -p r o o f gestational age) with improvement in COVID-19 pneumonia after treatment with C&I, resulting in successful vaginal delivery, along with a literature review.

Japanese medical care providers were facing the 5th COVID-19 epidemic (from the end of June through the end of September, 2021). On the August 20th, the maximum number of newly SARS-CoV-2-infected individuals reached 25,851/day. The Minami-Nagano Medical

Center was requested to accept the maternal transport of a 39-year-old pregnant female at 36 weeks and 6 days of gestation from a local hospital, who had already revealed positive results for the SARS-CoV-2 antigen test. The patient had a history of two uncomplicated vaginal deliveries and two spontaneous abortions without underlying diseases. She had not received a vaccination(s) against COVID-19. Her pregnancy was uneventful. Fever (more than 37C) as well as cough, malaise, and anorexia, occurred on August 25th, 2021. The patient was immediately admitted to our hospital six days later. Physical findings on admission showed a body temperature of 38.1°C, blood pressure of 98/60 mmHg, pulse rate of 60 beats/min, percutaneous saturation of oxygen (SpO2) 95% (under room air), and respiratory rate 18/min. Chest computed tomography images obtained on admission showed local distributions of infiltrations and ground-glass opacities in the subpleural areas of the bilateral lower lobes ( Fig.   1.) . The SpO2 (under room air) was approximately 93%. Her COVID-19 severity was judged to be moderate. C&I treatment was approved to attenuate the severe progression of COVID-19 under emergency use permission during the 5th epidemic in 2021. We expected that the C&I administration to this patient might prevent the severe progression of pneumonia.

On the other hand, we also considered the features of monoclonal antibody drugs in terms of J o u r n a l P r e -p r o o f pregnancy (including AU TGA and US FDA pregnancy categories) and lactation (Supplementary table 2) . After conducting the discussion regarding advantage (i.e., attenuation of disease severity) and disadvantage (e.g., AU TGA and US FDA pregnancy categories not available), we decided to treat her with C&I. We provided adequate verbal and written explanations to the patient/her husband and obtained written consent for the MAT administration. C&I was intravenously administered at a single dose for 50 min to reduce disease severity. No adverse reactions (including infusion reactions) were observed after the C&I administration.

On the second day of hospitalization, her fever gradually broke, along with a gradual resolution of cough, malaise, and anorexia (Fig. 2.) . The abdominal pain on admission was mild. Tests examining membrane rupture (Check PROM™) were negative. On the fifth day, however, the patient went into labor. The SpO2 (under room air) was gradually recovered (Fig.   2. ). These clinical manifestations suggested the improvement in COVID-19. We attempted to conduct vaginal delivery rather than cesarean section after considering the choice, since she was a full-term laboring woman without respiratory destress, and her last delivery was complete about 3 years. We brought her to a delivery room with negative pressure conditions, which had been originally built-in: all staff members in the room wore full personal protective after the water broke. Apgar scores were 8/8 at 1/5 min after birth. After delivery, her SpO2 was maintained at >95% (under room air). Fig. 2 . indicates the clinical course regarding perinatal patient. She required no oxygen supplementation during the perinatal period.

The neonate was isolated and separated from his mother. The newborn had a good and stable condition. Using nasopharyngeal specimens collected immediately after birth and 48 h later, the RT-loop-mediated isothermal amplification (LAMP) test (Loopamp™ SARS-CoV-2 Detection Kit) for detecting the RNA-dependent RNA polymerase/Nucleocapsid genes in the hospital, as well as the real-time RT-PCR test via the health center, were all negative. The newborn showed no signs (including fever or respiratory distress). The mother was placed in the same room with the newborn 10 days after her symptoms developed, and 3 days after her symptoms disappeared, and breastfeeding was started. She hugged her newborn 2 weeks after onset (when the mother's isolation period had expired). The patient and her newborn were discharged after the isolation period was completed. Thirty days after birth, the infant weighed 4.024 kg: the mother's pulmonary shadows had improved. The mother and infant had good health status.

Since the spread of the COVID-19 pandemic across Japan, we have accepted the J o u r n a l P r e -p r o o f hospitalization of more than 100 patients. Of these patients, 3 had a gestational age of 30 weeks or more; 2 cases (including this one) resulted in delivery during the treatment period against COVID-19. We performed a literature review of perinatal cases of COVID-19 in Japan [11] [12] [13] , along with the first report of a 37-week pregnant woman with COVID-19 pneumonia who delivered a male newborn through a cesarean section in 2020 [14] ( Table 1) .

We searched for related articles by entering keywords ''casirivimab, imdevimab, pregnant'' into the PubMed database (https://pubmed.ncbi.nlm.nih.gov/), and only one report described 2 cases of childbirth after treatment with C&I from the US in December 2021 [15] . This report documented that two moderate COVID-19 pregnant women (one in the second trimester and another in the third trimester) treated with C&I did not progress to severe disease and did not experience an adverse drug reaction. Additionally, in 4 case series of maternal MAT in pregnancy, there was no evidence of pregnancy complications or treatment failure: all patients avoided progression to severe disease and none required additional COVID-19-related medical visits and hospitalizations [16] . To the best of our knowledge, this is the first Japanese report where treatment with C&I attenuated the COVID-19 severity and led to successful vaginal delivery.

MAT agents have been administered to patients with rheumatoid arthritis for approximately 20 years. In contrast, interleukin (IL)-6 inhibitors have been shown to improve survival among severely ill patients with COVID-19 [17] . While etanercept (ETN), a TNF- J o u r n a l P r e -p r o o f inhibitor that is administered to treat patients with rheumatoid arthritis, has a low incidence of fetal transfer in humans [18] , infliximab (IFX) is transferable to fetuses since IFX is detected in the blood specimens of postnatal infants [19] . However, several epidemiological studies have revealed that TNF- inhibitors can be used safely and continued during the entire pregnancy period in limited cases [6] [7] [8] [9] . Placental C&I transfer, as well as their effects on intrauterine fetal exposure, are not yet known. Therefore, the outcomes of mothers and infants receiving MAT need to be monitored carefully for a long period.

COVID-19-associated pneumonia may become more severe during late pregnancy compared to the non-pregnant population [20, 21] . TARC is a C-C motif chemokine 17 responsible for trafficking T helper 2 cells into sites of allergic inflammation. Recent study [22] has suggested the role of serum TARC in allergic asthma via contributing to mast cell and eosinophilic inflammation. Her serum TARC level (47.5 pg/mL) on admission was low, suggesting severe progression. Serum TARC levels of 87.5 pg/mL or less are associated with severe situations [23] .

Casirivimab and imdevimab are large proteins with molecular weights of over 145,000 Da and 144,000 Da, respectively [24] (Supplementary table 2) . ETN are observed even when the administration of ETN or ADA is continued during lactation [18, 25] . C&I has similar molecular weights: drugs' excretion into breast milk is expected to be limited and small. Additionally, the drugs secreted into breast milk are likely to be destroyed in the infant's gastrointestinal tract; the absorption by infants and their impacts are expected to be minimal. C&I is expected to be used as beneficial administration, which may overcome the risks during lactation. Thus, we started breastfeeding for the newborn after the mother's isolation period had expired.

The risk of infection to newborn associated with vaginal delivery needs to be considered.

Recent study [26] has demonstrated unlikely SARS-CoV-2 transmission during vaginal delivery, since no virus particles were detected in vaginal swabs of the pregnant women. In this case, RT-LAMP and RT-PCR test results were negative for the newborn.

Additionally, because of the COVID-19-transmission possibility through breast milk or bottles, we did not start breastfeeding until her isolation period had finished. SARS-CoV-2 was not detected in the breast milk of mothers with COVID-19 in another report [14] ( Table  Figure Legends 

Update: Characteristics of symptomatic women of reproductive age with laboratory-confirmed SARS-CoV-2 infection by pregnancy status -United States

Higher severe acute respiratory syndrome coronavirus 2 infection rate in pregnant patients

Characteristics of women of reproductive age with laboratory-confirmed SARS-CoV-2 infection by pregnancy status -United States

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Adalimumab level in breast milk of a nursing mother

Unlikely SARS-CoV-2 transmission during vaginal delivery