Literature DB >> 34453934

Monoclonal antibody treatment of symptomatic COVID-19 in pregnancy: initial report.

Jonathan S Hirshberg¹, Emily Cooke², Megan C Oakes³, Anthony O Odibo³, Nandini Raghuraman³, Jeannie C Kelly³.

Abstract

Entities: Chemical

Mesh：

Substances：

Year: 2021 PMID： 34453934 PMCID： PMC8386136 DOI： 10.1016/j.ajog.2021.08.025

Source DB: PubMed Journal: Am J Obstet Gynecol ISSN： 0002-9378 Impact factor: 8.661

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Objective

Neutralizing monoclonal antibodies (mAbs) targeting the spike protein of SARS-CoV-2 have been shown to reduce disease progression and hospitalization in those at a high risk of disease progression. The United States Food and Drug Administration (FDA) provided emergency use authorization (EUA) for neutralizing mAbs in November 2020, which included a warning for pregnant and lactating women. Mounting evidence showing that COVID-19 has a disproportionate effect on pregnant women with higher rates of viral infection and disease severity prompted the inclusion of pregnancy as a criterion for mAb therapy in the United States earlier this year. Although other monoclonal antibodies and their transplacental passage have been well-studied in pregnancy, there are no data on the safety or efficacy of anti-spike protein neutralizing mAbs. To our knowledge, there is no previously published report of the treatment of COVID-19 with mAbs in pregnancy (PubMed, August 8, 2021; search terms: “Monoclonal antibody,” “pregnancy,” and “COVID-19”).

Study Design

These cases were collected as a part of a quality improvement project at a single academic medical center that was deemed exempt by the Human Research Protection Office. Pharmacy records were reviewed to identify patients who received the SARS-CoV-2 neutralizing antibodies between November 2020 and July 2021. The charts of these patients were reviewed in detail to extract COVID-19 and pregnancy-related data. The patients met strict FDA EUA criteria to be considered for mAb therapy. Clinical disease severity was based on the National Institutes of Health (NIH) classifications. The products used at our institution included bamlanivimab and casirivimab plus imdevimab, based on the availability at the time of treatment.

Results

We reviewed data from 813 patients who received mAb therapy at our institution during the study period. Of note, 4 of these patients were pregnant at the time of infusion, and the maternal ages ranged from 26 to 34 years; their gestational ages ranged from 11 to 32 weeks. In addition, 2 of the 4 patients were overweight and the other 2 were obese. All had symptomatic COVID-19 at the time of diagnosis and were confirmed positive based on nasopharyngeal polymerase chain reaction testing. Furthermore, 2 of the 4 patients met the FDA EUA criteria for therapy based on immunosuppressive conditions—one based on diabetes mellitus and the other (the fourth patient) based on body mass index (BMI). Two patients had moderate disease at the time of treatment and the others were categorized as mild. All patients received casirivimab plus imdevimab and tolerated the infusion without immediate complication. One patient experienced disease progression after mAb therapy, developing shortness of breath and thus meeting the NIH criteria for moderate disease. None of the 4 pregnant women required additional outpatient visits or hospitalizations related to their COVID-19 diagnosis. No abnormalities in anatomy or growth were identified on ultrasound or at the time of delivery for any of the pregnancies. Two patients are still pregnant at this time and have no additional pregnancy complications. One pregnancy ended in term vaginal delivery of a healthy neonate in the setting of pregnancy-related hypertension and another pregnancy ended in preterm delivery after maternal trauma in an unrelated event (Table ).

Table

Patient characteristics and outcomes

Patient	Age (y)	BMI (kg/m²)	Existing pregnancy complications	Gestational age at treatment (wk+d)	COVID-19 severity at treatment	Symptom day at time of mAb infusion	Worst COVID-19 severity after treatment	Additional COVID-19 care required	Pregnancy outcomes
Patient A	25	32.7	Diabetes, hypertension	11+1	Mild	2	Mild	None	Currently 25 wk pregnant
Patient B	34	27.8	Postsplenectomy	32+0	Moderate	8	Moderate	None	36-wk delivery of normally grown fetus; maternal trauma
Patient C	29	37.0	Obesity	31+3	Mild	4	Moderate	None	37-wk delivery of normally grown fetus; diagnosis of gestational hypertension
Patient D	24	29.4	Shingles	32+0	Moderate	2	Moderate	None	Currently 38 wk pregnant

BMI, body mass index; mAb, monoclonal antibodies.

Hirshberg. Monoclonal antibody treatment of symptomatic COVID-19 in pregnancy. Am J Obstet Gynecol 2021.

Patient characteristics and outcomes BMI, body mass index; mAb, monoclonal antibodies. Hirshberg. Monoclonal antibody treatment of symptomatic COVID-19 in pregnancy. Am J Obstet Gynecol 2021.

Conclusion

In this case series of maternal mAb therapy in pregnancy, we found no evidence of pregnancy complications or treatment failure. All 4 patients avoided progression to severe disease and none required additional COVID-19-related medical visits or hospitalizations. Anti-spike protein neutralizing antibodies are human immunoglobulin G1 kappa with unadulterated Fc receptors, which should allow for facilitated diffusion across the placenta, raising the concern for transplacental passage. However, there were no fetal effects noted in our small cohort. Given the ongoing severity of the COVID-19 pandemic, especially during pregnancy, more information regarding the safety and efficacy of neutralizing mAbs in pregnancy is vital.

3 in total

1. Update: Characteristics of Symptomatic Women of Reproductive Age with Laboratory-Confirmed SARS-CoV-2 Infection by Pregnancy Status - United States, January 22-October 3, 2020.

Authors: Laura D Zambrano; Sascha Ellington; Penelope Strid; Romeo R Galang; Titilope Oduyebo; Van T Tong; Kate R Woodworth; John F Nahabedian; Eduardo Azziz-Baumgartner; Suzanne M Gilboa; Dana Meaney-Delman
Journal: MMWR Morb Mortal Wkly Rep Date: 2020-11-06 Impact factor: 17.586

2. Update on Transplacental Transfer of IgG Subclasses: Impact of Maternal and Fetal Factors.

Authors: Toby Clements; Thomas F Rice; George Vamvakas; Sara Barnett; Megan Barnes; Beverly Donaldson; Christine E Jones; Beate Kampmann; Beth Holder
Journal: Front Immunol Date: 2020-09-11 Impact factor: 7.561

3. Bamlanivimab plus Etesevimab in Mild or Moderate Covid-19.

Authors: Michael Dougan; Ajay Nirula; Masoud Azizad; Bharat Mocherla; Robert L Gottlieb; Peter Chen; Corey Hebert; Russell Perry; Joseph Boscia; Barry Heller; Jason Morris; Chad Crystal; Awawu Igbinadolor; Gregory Huhn; Jose Cardona; Imad Shawa; Princy Kumar; Andrew C Adams; Jacob Van Naarden; Kenneth L Custer; Michael Durante; Gerard Oakley; Andrew E Schade; Timothy R Holzer; Philip J Ebert; Richard E Higgs; Nicole L Kallewaard; Janelle Sabo; Dipak R Patel; Matan C Dabora; Paul Klekotka; Lei Shen; Daniel M Skovronsky
Journal: N Engl J Med Date: 2021-07-14 Impact factor: 91.245

3 in total

6 in total

1. Sotrovimab Use for COVID-19 Infection in Pregnant Kidney Transplant Recipient.

Authors: Fatima AlKindi; Ahmad Chaaban; Mohammad Al Hakim; Yousef Boobes
Journal: Transplantation Date: 2022-02-04 Impact factor: 5.385

2. A real-world assessment of tolerability and treatment outcomes of COVID-19 monoclonal antibodies administered in pregnancy.

Authors: Mei H Chang; Kelsie Cowman; Yi Guo; Hongkai Bao; Peter S Bernstein; Inessa Gendlina; Priya Nori
Journal: Am J Obstet Gynecol Date: 2022-01-21 Impact factor: 10.693

Review 3. Vaginal delivery after improvement in COVID-19 by monoclonal antibody treatment: A case report and literature review.

Authors: Eisuke Ogawa; Hirohisa Goto; Hiroyasu Ushimaru; Akemi Matsuo; Satoshi Takeda; Ryohei Nishimura; Takaaki Hondo; Takashi Takahashi
Journal: J Infect Chemother Date: 2022-03-07 Impact factor: 2.065