Optimization of the use of anti-TB drugs based on in situ - - PowerPoint PPT Presentation

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Optimization of the use of anti-TB drugs based on in situ - - PowerPoint PPT Presentation

1 Optimization of the use of anti-TB drugs based on in situ pharmacokinetics Landry BLANC CNRS CBMN, UMR R 52 5248 48, Uni niversi sit de de Bor ordeaux, CGFB RIC RICAI 2019 - 17 17 Dc cembre 2019 2019 Lung lesions due to


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Optimization of the use of anti-TB drugs based on in situ pharmacokinetics

Landry BLANC

CNRS – CBMN, UMR R 52 5248 48, Uni niversi sité de de Bor

  • rdeaux, CGFB

RIC RICAI 2019 - 17 17 Déc écembre 2019 2019

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Lung lesions due to tuberculosis

Dartois V, Nat Rev Microbiol, 2014

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Lung lesions due to tuberculosis

Dartois V, Nat Rev Microbiol, 2014

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Lung lesions due to tuberculosis

Dartois V, Nat Rev Microbiol, 2014

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Attenuation of antibiotic bactericidal activity on non-replicating bacteria

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Anti tibiotic ic *M *MBC90

90 in

rep eplicating cu cult lture (μM) M) Wayne mod

  • del

MBC BC90

90 (μM)

M) Lob Lobel l Model MBC BC90

90 (μM)

M) Case Caseum MBC BC90

90 (μM)

M) Rifampin 0.078 2 2 8 Isoniazid 0.31–0.63 >128 >128 >128 Pyrazinamide >80 >8,192 >8,192 512 Moxifloxacin 0.31–0.63 10 >128 2 Linezolid 10 >128 >128 128 Kanamycin 5.0 >128 80 >128 Clofazimine 40 >128 >128 >128 Bedaquiline 10 >20 >20 32 Rifapentine 0.078 0.5 10 2 Rifabutin 0.039 0.5 10 2

* Minimum Bactericidal Concentration

Sarathy et al, Extreme Drug Tolerance of Mycobacterium tuberculosis in Caseum, AAC, 2018

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How to study and quantify drugs penetration in tuberculosis lesions ?

  • Lesions dissection coupled with LC-MS/MS
  • Laser Capture Microdissection (LCM) combined

with LC-MS/MS

  • MALDI* Mass Spectrometry Imaging (MSI)

6 * * Matr trix ix-As Assis isted Laser Des esorptio tion/Ioniz izatio tion

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Lesions dissection coupled with LC-MS/MS

Fully quantitative Highly sensitive and selective for the drugs of interest Poor spatial information

Limited to the size of the original homogenized tissue

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Lesions dissection Homogenization Chemical extraction and inactivation

Uninvolved lung tissues (UI) Tissue surrounding the lesions (SL), Cellular Lesions (LE), Wall of Cavitary lesions (CAW) Cavitary Caseum and Necrotic Center (CAC/NC).

Dalin Rifat et al, STM, 2018

LC/MS/MS Quantification

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Laser Capture Microdissection (LCM) combined with LC-MS/MS

8 Zimmerman & al, JOVE, 2018

Sn Snap frozen sample Gamma irradiation Se Sectionning Extrac acti tion LC LC/M /MS/MS Quan uanti tification Diss ssection

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  • Fully quantitative capabilities
  • Sensitivity of the LC/MS analysis
  • Spatially-resolved quantification
  • Blind dissection

Laser Capture Microdissection (LCM) combined with LC-MS/MS

9 Zimmerman & al, JOVE, 2018

Sn Snap frozen sample Gamma irradiation Se Sectionning Extrac acti tion LC LC/M /MS/MS Quan uanti tification Diss ssection

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Ethambutol penetration in infected rabbit studied by LCM-LC/MS

  • Steady state dosing : daily shot (100 mg/kg) during 1 week
  • Ethambutol reaches the required dose to elimate bacteria in each

granuloma compartment

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*

*Intramacrophagic Minimal Bacteriocidal Concentration

Zimmerman & al, AAC, 2017

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  • Regular MALDI mass spectrometry on each individual pixel (1 spectrum = 1pixel)
  • Multiple pixels acquisition allows to build a map for each detected peak

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Römpp et al., Histochem. Cell Biol., 2013, 139, 759-789

MALDI Mass Spectrometry Imaging (MSI): Principle

Mat atrix ix-Assis isted La Laser Des esorptio ion/Ioniz izatio ion

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MALDI Mass Spectrometry Imaging: Workflow

1) Snap frozen Gamma irradiated sample 2) Cryo-sectioning and thaw- mounting on slide 4) Matrix application (sprayer / sublimation chamber) 5) AP-MALDI5 AF – Orbitrap Hi High mas ass re resolu lutio ion 8) Alignement with histological image 7) Data processing 6) AP-MALDI5 AF – Orbitrap spectrum 3) Sample preparation 3a) Lipids, drugs metabolites, small molecules… 3b) Peptides/Proteins 3c) Glycans/Polysaccharides

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High-resolution mapping of fluoroquinolones in TB rabbit lesions reveals specific distribution in immune cell types.

Penetration of fluoroquinolones in granuloma seems following a pattern

This pattern could correspond to layer of different cell type

Rabbit 1063 – 2h Rabbit 2069 – 6h

MXF LVX GTX

2 mm 2 mm 2 mm

N N N

E

Uninvolved lung Mac acrophages Lymphocytes Foa

  • amy

y Mac acrophages Caseum

c

2 mm

c

13 L.Blanc et al, eLife, 2018

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Regions of Interest highlighting moxyfloxacin distribution defined by MALDI MSI and transposed on histological image

14 L.Blanc et al, eLife, , 2018

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Mathematical model of moxyfloxacin distribution to decipher key parameters driving it

  • Histopatholigical evaluation of cell

populations in the different areas

  • % macrophage
  • % lymphocyte
  • % necrotique
  • % neutrophile

5 10 15 20 25 30 MXF LVX GTX

intracellular/extracellular concentration ratio

Macrophages Lymphocytes Neutrophils Epithelial cells **** * * *** * * *** * *

In vitro validation : drug uptake in different cell lines

2 1 1 7 1 2 7 1 8 1 5 1 4 2 0 3 1 2 5 2 7 2 8 3 3 4 8 3 2 2 4 2 9 9 1 6 1 3 1 9 3 3 3 0 3 5 2 2 6 4 2 6 2 3 5 1 0 2 1 1 1 0 .0 0 0 .0 2 0 .0 4 0 .0 6

MXF signal normalized to internal standard (pixel intensity)

Computer modeling

3 Key parameters : Di Distance from granuloma edge ↘ Percentage of macrophage ↗ Percentrage of necr necros

  • sis

is ↘

15 L.Blanc et al, eLife, , 2018

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Distribution study of clofazamine with high resolution MSI

500 µm

Pixel size: 50 µm Pixel size: 15 µm Pixel size: 5 µm

High spatial resolution with AP- SMALDI5-Orbitrap (TransMIT) Spatial resolution down to 5µm coupled with high resolution mass spectrometer

Pixel size down to cellular level

Very precise scan of clofazamine distribution

Alignment of HE and MSI image to reveal clofazamine accumulation in macrophage Reaching foamy macrophage But limited penetration in necrotic core

Granuloma in infected mice Treated daily with CFZ during 1 month

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TB Granuloma is a poorly vascularized region where drug penetration is complex Moreover, an extreme drug tolerance of Mycobacterium tuberculosis could be

  • bserved in caseum

Cidal activity of most drugs is less efficient on non-replicating bacterias

Drug exposure and MBC in situ are key factors Different mass spectrometry techniques are suitable for PK studies:

LC/MS quantification on regular dissected tissue

Sensitive and fully quantitative But limited in term of spatial information

Laser Capture Microdissection coupled with LC/MS

Sensitive and fully quantitative Investigation at granuloma structure level, but blind dissection

Mass Spectrometry Imaging

Less sensitive and semi quantitative Very valuable spatial information (cellular level)

Combination of both techniques for LCM guided by Mass Spectrometry Imaging

Take home message…

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Acknowledgment

Véronique Dartois Nicolas Desbenoit Caroline Tokarski Brendan Prideaux

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THANK YOU FOR YOUR ATTENTION

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