# Recombinant Ixodes scapularis Calreticulin Binds Complement Proteins but Does Not Protect Borrelia burgdorferi from Complement Killing

**Authors:** Moiz Ashraf Ansari, Thu-Thuy Nguyen, Klaudia Izabela Kocurek, William Tae Heung Kim, Tae Kwon Kim, Albert Mulenga

PMC · DOI: 10.3390/pathogens13070560 · 2024-07-03

## TL;DR

This study explores how a tick protein interacts with human complement proteins but does not protect Lyme disease bacteria from immune attack.

## Contribution

The novel finding is that recombinant tick calreticulin binds complement proteins but does not protect Borrelia burgdorferi from complement killing.

## Key findings

- Recombinant Ixodes scapularis calreticulin binds to C1 complex and intermediate complement proteins.
- Despite binding, it does not protect Borrelia burgdorferi from complement-induced killing.
- rIxsCRT promotes B. burgdorferi replication in culture.

## Abstract

Ixodes scapularis is a blood-feeding obligate ectoparasite responsible for transmitting the Lyme disease (LD) agent, Borrelia burgdorferi. During the feeding process, I. scapularis injects B. burgdorferi into the host along with its saliva, facilitating the transmission and colonization of the LD agent. Tick calreticulin (CRT) is one of the earliest tick saliva proteins identified and is currently utilized as a biomarker for tick bites. Our recent findings revealed elevated levels of CRT in the saliva proteome of B. burgdorferi-infected I. scapularis nymphs compared to uninfected ticks. Differential precipitation of proteins (DiffPOP) and LC-MS/MS analyses were used to identify the interactions between Ixs (I. scapularis) CRT and human plasma proteins and further explore its potential role in shielding B. burgdorferi from complement killing. We observed that although yeast-expressed recombinant (r) IxsCRT binds to the C1 complex (C1q, C1r, and C1s), the activator of complement via the classical cascade, it did not inhibit the deposition of the membrane attack complex (MAC) via the classical pathway. Intriguingly, rIxsCRT binds intermediate complement proteins (C3, C5, and C9) and reduces MAC deposition through the lectin pathway. Despite the inhibition of MAC deposition in the lectin pathway, rIxsCRT did not protect a serum-sensitive B. burgdorferi strain (B314/pBBE22Luc) from complement-induced killing. As B. burgdorferi establishes a local dermal infection before disseminating to secondary organs, it is noteworthy that rIxsCRT promotes the replication of B. burgdorferi in culture. We hypothesize that rIxsCRT may contribute to the transmission and/or host colonization of B. burgdorferi by acting as a decoy activator of complement and by fostering B. burgdorferi replication at the transmission site.

## Linked entities

- **Proteins:** C1qa (complement component 1, q subcomponent, alpha polypeptide), C1R (complement C1r), C1S (complement C1s), C3 (complement C3), C5 (complement C5), C9 (complement C9), yip7 (yippee interacting protein 7)
- **Diseases:** Lyme disease (MONDO:0019632)
- **Species:** Ixodes scapularis (taxon 6945)

## Full-text entities

- **Genes:** CALR (calreticulin) [NCBI Gene 811] {aka CALR1, CRT, HEL-S-99n, RO, SSA, cC1qR}
- **Diseases:** infection (MESH:D007239), tick bites (MESH:D064927), LD (MESH:D008193)
- **Species:** Ixodes scapularis (blacklegged tick, species) [taxon 6945], Borreliella burgdorferi (Lyme disease spirochete, species) [taxon 139], Saccharomyces cerevisiae (baker's yeast, species) [taxon 4932], Homo sapiens (human, species) [taxon 9606]
- **Cell lines:** B314 — Cricetulus griseus (Chinese hamster), Hybrid cell line (CVCL_1R86)

## Figures

11 figures with captions in the complete paper: https://tomesphere.com/paper/PMC11280304/full.md

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Source: https://tomesphere.com/paper/PMC11280304