There is no risk of infertility from COVID-19 vaccines due to cross-reactivity with placenta proteins, as SARS-CoV-2 and placenta proteins are different

CLAIM
“Covid Vaccine is Female Sterilization”; SARS-CoV-2 vaccines may trigger an immune response against the placenta.
DETAILS
Factually Inaccurate: It is inaccurate to claim that COVID-19 vaccines cause female infertility or that the SARS-CoV-2 Spike protein and the human protein syncytin-1 are very similar. These two proteins only have very short sequences of amino acids in common. This is not specific to the SARS-CoV-2 Spike protein as syncytin-1 also shares short sequences with many other proteins.
Flawed reasoning: If there was a risk of an immune response reacting against both the SARS-CoV-2 Spike protein and the human protein syncytin-1, which plays a role in placenta function, then women who had COVID-19 would be sterile. However, such an effect of COVID-19 has not been reported. Furthermore, given that short segments of protein sequences are shared by syncytin-1 and the Spike proteins of common cold coronaviruses, a peak of infertility should be observed every winter, but this is not the case.
KEY TAKE AWAY
Frontrunner COVID-19 vaccines have been found safe during Phase III clinical trials enrolling dozens of thousands of patients. Claims of vaccine induced infertility due to the presence of SARS-CoV-2 proteins in them are illogical as we would then see a peak of infertility among COVID-19 patients or during winter when many people get infected by other, benign, coronaviruses. The viral proteins contained in the vaccines are different from the proteins present in our body.

FULL CLAIM: “Covid Vaccine is Female Sterilization”; “the vaccine contains a Spike protein called syncytin-1”; “we are also training the female body to attack syncytin-1, which could lead to infertility”

REVIEW


The COVID-19 pandemic motivated unprecedented efforts to develop vaccines against SARS-CoV-2, the virus responsible for the disease. Towards the end of 2020, several vaccine candidates reached the approval phase. However, the rollout of these vaccines has been accompanied by many unsupported allegations about their dangers.

One of these claims originated from an open letter written by physician Wolfgang Wodarg and Michael Yeadon, a former employee of Pfizer. The two alleged that the virus SARS-CoV-2 and the human placenta produce similar proteins, specifically, the viral Spike protein and the human protein syncytin-1. Syncitin-1 allows placenta cells to fuse together and is a crucial protein for the correct development of the placenta and a successful pregnancy. Therefore, when a woman gets vaccinated against COVID-19, her immune system would learn to detect the Spike protein contained in the vaccine but would also detect and attack the placenta protein syncytin-1, due to a phenomenon called cross-reactivity.

A person’s immune system responds to disease-causing microorganisms (pathogens) by recognizing specific “patterns” on pathogens, such as segments in their protein sequences. A cross-reactivity occurs when cells or antibodies are able to detect and destroy multiple targets based on similarities in their protein sequences.

Contrary to the claim, the SARS-CoV-2 Spike protein and the human protein syncytin-1 are not similar in terms of their composition in amino acids.

A database search of the human genome for proteins homologous to the Spike protein of SARS-CoV-2 returned no matches at all, demonstrating the lack of similarities between the two proteins. François Balloux, a geneticist at University College London, explained on Twitter that the comparison of syncytin-1 and SARS-CoV-2 yielded “no sequence homology”. Two proteins are said to be homologous when their similarities of sequence are significant indicating that they are evolutively related.

Yeadon later clarified that his claim was based on a small sequence of five amino acids, of which four are shared between syncytin-1 and the SARS-CoV-2 Spike protein. However, Balloux explains that similarities between the two proteins in a small number of amino acid sequences is insufficient to trigger a cross-reaction of the immune system. A minimum of 8 matching amino acids would be required to have a good chance (or risk) of cross-reactivity.

Second, the “4 out of 5” matching sequence mentioned by Yeadon is so short that one could find comparable matches between the SARS-CoV-2 Spike protein and many other human proteins, not just syncytin-1. Immunologist Andrew Croxford compared the protein sequence of the SARS-CoV-2 Spike protein to proteins that are present at high levels in the human body. He found another “4 out of 5” matching sequence between the Spike protein and another human protein called actin. He also found a “4 out of 6” matching sequence with human collagen and a “5 out of 6” matching sequence with human hemoglobin. Frederik Lermyte, a biochemist at the Technical University of Darmstadt ran similar comparisons and also concluded that there is no meaningful similarity between the SARS-CoV-2 Spike protein and syncytin-1.

The bottom line is that a sequence of four or five amino acids is so short that it is likely to occur in many proteins. The three proteins analyzed by Croxford are absolutely vital for the functioning of our body. Actin is an essential component of muscles and participates in their contraction. Collagens are necessary to maintain the structure of our tissues and hemoglobin is responsible for the transport of oxygen in Red Blood Cells. If such small matching sequences where sufficient to trigger a cross reactivity between SARS-CoV-2 Spike and those proteins, then many people who had COVID-19 or who are participating in the vaccine clinical trials would likely have developed an autoimmune response against their own actin, collagen, or hemoglobin, with significant disorders.

Another argument that counters the idea of immune system cross-reactivity between the SARS-CoV-2 Spike protein and syncytin-1 is that the Spike protein is present in all coronaviruses. Four of these coronaviruses, named 229E, NL63, OC43, and HKU1, are responsible for the common cold. Therefore, many humans have already been in contact with at least one of them. These common cold coronaviruses also share similarities of very short sequences of four or five identical amino acids with human syncytin-1, see Figure 1 and 2 for examples. Yet, infections with these common cold coronaviruses don’t trigger an autoimmune response that destroys the human placenta. If this were the case, we would observe a peak of female infertility every winter.


Figure 1: Short similarity between human syncytin-1 and the Spike protein from the common cold coronavirus 229E. This is an alignment between a fragment of the syncitin-1 protein (starting at amino acid number 354) and the 229E Spike protein (starting at amino acid 812). The letters indicate the type of amino acid encountered at each position. Asterisks indicate the presence of an identical amino acid between the two proteins. The red rectangle highlights a stretch of five amino acids where three are identical between the two proteins.


Figure 2: Short similarity between human syncytin-1 and the Spike protein from the common cold coronavirus NL63. This is an alignment between a fragment of the syncitin-1 protein (starting at amino acid number 144) and the NL63 Spike protein (starting at amino acid 1239). The letters indicate the type of amino acid encountered at each position. Asterisks indicate the presence of an identical amino acid between the two proteins. The red rectangle highlights a stretch of six amino acids where five are identical between the two proteins.

In summary, the similarities between the SARS-CoV-2 Spike protein and the human placenta protein syncytin-1 are extremely small. Such similarities are present in many other proteins, but do not trigger broad autoimmune responses among COVID-19 patients. Similarities between syncytin-1 and the Spike protein of the common cold coronaviruses can also be detected, and yet no seasonal infertility is recorded, which would have been the case if brief identical sequences were sufficient to trigger immune cross-reactivity. It is true that clinical trials from the vaccine frontrunners tend to exclude pregnant women from the cohorts, which creates a gap in our knowledge that needs to be filled. However, it is inaccurate to claim that syncytin-1 and SARS-CoV-2 Spike protein are very similar. Furthermore, it is extremely unlikely that a person’s exposure to the SARS-COV-2 Spike protein via a COVID-19 vaccine would trigger an autoimmune response against the placenta.

READ MORE

An in-depth analysis showing the lack of homology between syncytin-1 and the viral Spike protein. The author lists additional arguments, such as the fact that for cross-reactivity to occur, there must be more than one short identical sequence between two proteins.

UPDATE (21 Dec. 2020)

The headline of the article was updated for clarity.

     

Published on: 10 Dec 2020 | Editor:

Health Feedback is a non-partisan, non-profit organization dedicated to science education. Our reviews are crowdsourced directly from a community of scientists with relevant expertise. We strive to explain whether and why information is or is not consistent with the science and to help readers know which news to trust.
Please get in touch if you have any comment or think there is an important claim or article that would need to be reviewed.

ifcn-fact-checkers-code-of-principles-signatory