The Small Breathing Amplitude at the Upper Lobes Favors the Attraction of Polymorphonuclear Neutrophils to Mycobacterium tuberculosis Lesions and Helps to Understand the Evolution toward Active Disease in An Individual-Based Model
Authored by Pere-Joan Cardona, Clara Prats
Date Published: 2016
DOI: 10.3389/fmicb.2016.00354
Sponsors:
No sponsors listed
Platforms:
NetLogo
Model Documentation:
ODD
Flow charts
Model Code URLs:
Model code not found
Abstract
Infection with Mycobacterium tuberculosis (Mtb) can induce two kinds of
lesions, namely proliferative and exudative. The former are based on the
presence of macrophages with controlled induction of intragranulomatous
necrosis, and are even able to stop its physical progression, thus
avoiding the induction of active tuberculosis (TB). In contrast, the
most significant characteristic of exudative lesions is their massive
infiltration with polymorphonuclear neutrophils (PMNs), which favor
enlargement of the lesions and extracellular growth of the bacilli. We
have built an individual-based model (IBM) (known as ``TBPATCH{''})
using the NetLogo interface to better understand the progression from
Mtb infection to TB. We have tested four main factors previously
identified as being able to favor the infiltration of Mtb-infected
lesions with PMNs, namely the tolerability of infected macrophages to
the bacillary load; the capacity to modulate the Th17 response; the
breathing amplitude (BAM) (large or small in the lower and upper lobes
respectively), which influences bacillary drainage at the alveoli; and
the encapsulation of Mtb-infected lesions by the interlobular septae
that structure the pulmonary parenchyma into secondary lobes. Overall, although all the factors analyzed play some role, the small BAM is the
major factor determining whether Mtb-infected lesions become exudative, and thus induce TB, thereby helping to understand why this usually takes
place in the upper lobes. This information will be very useful for the
design of future prophylactic and therapeutic approaches against TB.
Tags
Infection
Mechanisms
Granuloma-formation
Protocol
Mice
Cell
Alveolar macrophages
Secondary