key: cord-1039012-mx4xc0ou
authors: Edward Uzoigwe, Chika
title: Body temperature and host species preferences of SARS-CoV-2
date: 2020-07-17
journal: Clin Microbiol Infect
DOI: 10.1016/j.cmi.2020.07.017
sha: bcc92c8f37895347f87604c86d9a8930ac0cc14e
doc_id: 1039012
cord_uid: mx4xc0ou

nan

1

Harcourt House Sheffield chika@doctors.org.uk Tel: 07527907618

To the Editor There is currently uncertainty regarding the zoonotic repertoire of SARS-CoV-2. Shi et al. observed that cats were susceptible. Dogs and ferrets show intermediate vulnerability. The pathogen failed to infect or replicate in pigs, chickens, and ducks [1] . Their data strongly suggests that the pathogen's species predilection may be related to body temperature. The preferred hosts, human and cats, exhibit mean body temperatures, below that of more resistant hosts such as pigs, chicken and ducks (table 1) , whose corporal temperatures can range between 39 o C and 42 o C (table 1) .

A similar pattern has been observed with the suspected hosts, South East Asian bats, the Chinese pangolin and masked palm civets (Paguma larvata); all modest corporal temperature hetero and homeo-therms (Table 1) . Bats do show considerable diurnal and seasonal variation in body temperature, notably with precipitous drops during periods of torpor and hibernation. This may render them an idonaeous host to act as a viral reservoir.

In addition, of the note, Shi et al reported that SARS-CoV-2 infectious virions were only isolated in their upper airways but not in other viscera following inoculation [1] . Further the virus was only able to replicate in the upper respiratory tract [Error! Bookmark not defined.]. This is notwithstanding the fact the docking ACE2 enzyme-receptor is located throughout the airways and lungs of ferrets. Indeed ex vivo SARS-CoV-2 did bind to ferret bronchiolar cells [1] . It is noteworthy that the ferret holds a somewhat intermediate core temperature, higher than that of favoured host, humans and cats but less than that of pigs and ducks (table 1) . Clearly the upper airways are at a lower temperature than core temperature, potentially explaining the predisposition of SARS-CoV-2 for the upper respiratory tract.

The European mink has been found to be also vulnerable to SARS-CoV-2, with significant animal attrition observed In two mink farms in the Netherlands due to the virus [2] . Tellingly the European mink has recorded corporal temperatures of between 36.2 o C and 38.4 o C (Table 1 ).

In further support of this SARS-CoV-2 temperature phenomenon, the virus has been shown to be exquisitely temperature labile, more so than ancestral SARS-CoV-1. Ou et al. demonstrated the S surface protein of SARS-CoV-2, responsible for binding to ACE2, to be particularly temperaturesensitive, with activity dropping precipitously as temperatures rise above 37.5 o C3.

Interestingly Wan et al found pig, ferret and cat ACE2 to be identical or very similar to human ACE2 at "critical virus binding residues" [4] . However Shi et al. showed only the cat to be an unequivocal host[Error! Bookmark not defined.]. Pig ACE2 shows greater homology to human ACE2 than either that of cats and ferrets but only the latter two were shown to be hosts [1, 4] . Further cat and ferret ACE are identical at critical viral-binding residues and yet the cat is a permissive host and the ferret only partially vulnerable. Hence species affinity of SARS-CoV-2 cannot be explained exclusively ACE2 morphology.

The temperature lability of SARS-CoV-2 may be germane to immune evasion. Ou et al showed that the S protein of both SARS-CoV 1 and 2 were deactivated even at temperatures of 37 o C [3] . The S protein of SARS-CoV-2 was much more susceptible to this deactivation than that of SARS-CoV-1. The fleeting existence of the protein in the blood at these temperatures, prior to denaturation, may prevent the host from mounting a comprehensive immune response. Alternatively, seroconversion may occur to an S protein altered by thermo-degradation and thereby a quasi-decoy antigen. A recent statement from the World Health Organisation suggests that infection does not necessarily confer immunity even with the detection of antibodies [https://www.who.int/newsroom/commentaries/detail/immunity-passports-in-the-context-of-covid-19]. Questions remain regarding immunity following infection [5] . Further preliminary evidence from the US Centre for Disease Control and Prevention shows that those infected mount a much more consistent IgA than IgG response; indicative of epithelial surface-centred rather than serum-centred immunity[https://wwwnc.cdc.gov/eid/article/26/7/20-0841_article]. Evidence points to a nascent but rather inchoate immune response to SARS-CoV-2, potentially truncated by temperature vulnerability of the spike protein.

In summary, temperature lability of SARS-CoV-2 S-protein may limit its host repertoire but equally may truncate pathogen exposure to host immunity, curtailing the amplificative catenation of cellular and molecular events involved in primary immunity. 

Susceptibility of ferrets, cats, dogs, and other domesticated animals to SARS-coronavirus 2

SARS-CoV-2 infection in farmed minks, the Netherlands

Characterization of spike glycoprotein of SARS-CoV-2 on virus entry and its immune cross-reactivity with SARS-CoV

Receptor Recognition by the Novel Coronavirus from Wuhan: an Analysis Based on Decade-Long Structural Studies of SARS Coronavirus

COVID-19 and Postinfection Immunity: Limited Evidence, Many Remaining Questions