An Insight from the Tebubio Team
Tebubio offers a comprehensive toolbox to explore lysosomal function, all compatible with microscopy, plate readers, and flow cytometry.
Easy & ready assays to implement, our solutions are designed to help you generate reliable, reproducible data without requiring specialised instrumentation. Looking for tailored approaches?
Lysosomes Unveiled: Advanced Tools and Insights
For decades, lysosomes were simplistically regarded as mere “waste disposal” units of the cell. However, a wealth of recent research has dismantled this outdated perception. Today, lysosomes are recognised as dynamic organelles at the heart of numerous essential cellular processes, including homeostasis, signalling, immunity, and disease progression.
As the scientific community delves deeper into lysosomal biology, the demand for precise and reliable tools to investigate lysosomal function and dysfunction has never been greater. Whether the focus is on neurodegeneration, cancer, or fundamental cell biology, understanding lysosomes opens a gateway to novel therapeutic strategies and deeper biological insights.
Explore this article
Lysosomal Dysfunction: A Common Denominator in Diverse PathologiesThe Lysosome: A Multifunctional Cellular Hub
Deciphering Lysosomal Function: A Suite of Innovative Assays
Probing Lysosomal Acidification: Targeting v-ATPase Activity
Cathepsins and LAMPs: Unravelling Lysosomal Identity and Functionality
Need to Go Further? We’ve Got You Covered
From Lysosomal Function to Disease Mechanisms: Let’s Talk Science
Lysosomal Dysfunction: A Common Denominator in Diverse Pathologies
Lysosomes have emerged as central players in several pathological mechanisms. In Alzheimer’s disease, impaired lysosomal acidification hinders the clearance of amyloid-beta, leading to the accumulation of autophagic vacuoles and the notorious formation of neurotoxic plaques [(PubMed ID: 35654956)].
Conversely, in the context of cancer, lysosomes contribute to both cellular demise and tumour propagation. Dysregulated lysosomal iron levels can instigate lipid peroxidation, triggering ferroptosis, a non-apoptotic cell death pathway, that holds promise for eliminating treatment-resistant cancer cells [(PubMed ID: 38659936)]. Learn more about ferroptosis in our dedicated blog post: "Ferroptosis Decoded: Tools and Insights to Unravel Iron-Driven Cell Death".
In parallel, lysosomes are tightly linked to reactive oxygen species (ROS) metabolism, as their activity modulates oxidative stress responses and redox homeostasis within cells. Disruptions in lysosomal function can exacerbate ROS generation, creating a vicious cycle implicated in both degenerative diseases and cancer progression. For a deep dive into ROS and its role in cellular dysfunction, read our ROS-focused blog post: "Rethinking ROS Detection: A New Era for Redox Biology Research".
Simultaneously, lysosomes remodel the tumour microenvironment, fostering invasion and metastasis [(PubMed ID: 33718382)].
Such multifaceted roles position lysosomes as pivotal determinants of both disease evolution and therapeutic outcomes.
The Lysosome: A Multifunctional Cellular Hub
Fundamentally, lysosomes are acidic, membrane-bound organelles tasked with degrading and recycling cellular waste, encompassing extracellular material via endocytosis and phagocytosis, and intracellular components through autophagy. The degradation products are either recycled within the cell or expelled through lysosomal exocytosis, as illustrated in Figure 1.
Figure 1: Schematic overview of the lysosomal pathway.
Beyond degradation, lysosomes orchestrate a variety of cellular functions, including calcium signalling, nutrient sensing, plasma membrane repair, redox balance, and even regulation of cell migration. Notably, lysosomal morphology and distribution vary across cell types, with specialised tubular lysosomes frequently observed in antigen-presenting cells such as macrophages and dendritic cells.
These diverse functionalities underpin the necessity for robust, versatile tools to dissect lysosomal biology across multiple experimental models.
Deciphering Lysosomal Function: A Suite of Innovative Assays
Recognising the diverse needs of researchers, Tebubio offers lysosomal function kits tailored to investigate specific aspects of lysosomal biology in live-cell models:
Lysosomal Function Kits
|
Description |
Product Name |
Reference |
Highlights |
| Autophagy (Autolysosome) Detection | DALGreen-Autophagy Detection | D675-10 | Detect Autolysosome selectively in Live Cells |
| Lysosomal Quantity Detection (Green) | LysoPrime Green-High Specificity and pH Resistance | L261 |
pH-independent/resistant, with high retention activity (Figure 2) |
| Lysosomal Quantity Detection (Deep Red) | LysoPrime Deep Red-High Specificity and pH Resistance | L264 | pH-independent/resistant, with high retention activity (Figure 3) |
| Lysosomal Acidic pH Detection (Red) | pHLys Red-Lysosomal Acidic pH Detection | L265 | pH-dependant |
| Lysosomal Acidic pH Detection Kit (L261 + L265) | Lysosomal Acidic pH Detection Kit | L266-10 | Simultaneously, analysis of lysosomal mass and pH |
| Lysosomal Acidic pH Detection Kit (L264 + pHLys Green) | Lysosomal Acidic pH Detection Kit | L268-10 | Simultaneously, analysis of lysosomal mass and pH |
| Lysosomal staining in live cells | SiR-Lysosome kit | SC012 | Standard Cy5 filter sets |
| Lysosomal staining in live cells | SiR700-lysosome kit | SC016 | Standard Cy5 filter sets |
| Lysosomal membrane tension probe | Lyso Flipper-TR® | SC022 | Monitor changes in membrane tension by changing its fluorescence lifetime as a function of the twist between its fluorescent groups |
Figure 2: Superior Lysosomal Labelling with LysoPrime Green. Overcoming pH-Dependent Staining and Enhancing Long-Term Imaging Reliability.
Figure 3: Disrupting Vesicle-Lysosome Fusion Dynamics. Co-labelling with ECGreen, LysoPrime Deep Red, and pHLys Red Reveals Bafilomycin A1-Mediated Inhibition of Lysosomal Acidification and Fusion Events.
The ability to accurately visualise lysosomal dynamics, independent of pH fluctuations or probe instability, is essential for studying processes such as vesicle trafficking, autophagic flux, and organelle fusion events. Figures 2 and 3 illustrate how advanced probes like LysoPrime Green, LysoPrime Deep Red, and pHLys Red enable precise, long-term monitoring of lysosomal mass and acidification, overcoming the limitations of traditional dyes.
These tools not only enhance imaging fidelity but also provide researchers with robust solutions to dissect complex lysosomal functions in real-time, whether analysing membrane tension, tracking lysosome-endosome fusion, or investigating the impact of inhibitors such as Bafilomycin A1 on lysosomal activity.
Such refined methodologies are crucial for understanding lysosome-related mechanisms in pathological contexts like neurodegeneration, cancer, ferroptosis, and oxidative stress (ROS), where lysosomal dysfunction is often a key driver.
Probing Lysosomal Acidification: Targeting v-ATPase Activity
A defining feature of lysosomes is their acidic luminal environment, maintained by the v-ATPase complex, which utilises ATP hydrolysis to pump protons into the organelle. Perturbations in this delicate proton balance are directly implicated in disease phenotypes.
For functional studies aimed at modulating lysosomal pH, Tebubio provides a comprehensive portfolio of v-ATPase inhibitors:
|
Product Name |
Reference |
|---|---|
| Bafilomycin A1 | T6740 |
| Bafilomycin B1 | |
| Bafilomycin C1 | |
| Bafilomycin D | BIA-B1162 |
| Concanamycin A |
Figure 4: Properties of the lysosome.
Inhibiting v-ATPase not only serves as a tool to dissect lysosomal acidification mechanisms but also aids in studying the interplay between lysosomal positioning, pH gradients, and cellular trafficking (Figure 4).
Cathepsins and LAMPs: Unravelling Lysosomal Identity and Functionality
Lysosomes are equipped with over 70 hydrolases, among which cathepsins hold particular relevance. These proteases are integral to antigen processing, bone remodelling, hormone activation, and pathological processes, including cancer metastasis and neuroinflammation. Tebubio offers a selection of cathepsin inhibitors and specialised kits for quantifying cathepsin activity across various species and sample types.
Complementing the luminal enzymes, lysosomal-associated membrane proteins (LAMP1 and LAMP2) represent key structural components vital for maintaining lysosomal integrity and mediating vesicle fusion events. However, to accurately distinguish lysosomes from late endosomes, markers such as CD63 are indispensable.
Tebubio provides a targeted suite of detection reagents, including:
|
Description |
Product Name |
Reference |
Highlights |
| Primary antibodies | Human LAMP1 antibodies | Access the products | Cell samples |
| Primary antibodies | LAMP2 antibodies | Access the products | Cell samples |
| ELISA kits, NexaTag™ qIPCR ELISA kits |
LAMP1 and LAMP2 quantification kits | Access the products | Serum, plasma, and cell culture supernatant samples. |
| Primary antibodies | Human CD63 antibodies | Access the products | Cell samples |
Need to Go Further? We’ve Got You Covered
Whether you're delving into lysosomal biology for the first time or planning advanced functional studies, Tebubio offers more than just reagents; we provide comprehensive solutions. Our portfolio includes ready-to-use probes, assays, and modulators designed specifically for lysosomal research, as well as Contract Research Services tailored to your experimental models and scientific objectives.
From assay optimisation and high-content screening to protocol development and sourcing of specialised compounds, our team of Project Managers is ready to support you at every stage of your project.
Let’s co-design your next breakthrough in lysosomal research.
From Lysosomal Function to Disease Mechanisms: Let's Talk Science
Whether your research focus is to decode lysosomal trafficking pathways, monitor autophagic flux, or interrogate lysosomal contributions to disease pathology, Tebubio’s expert team is here to support you.
Our Product Managers are available to provide tailored advice, suggest optimal experimental workflows, and assist you in selecting the most appropriate reagents for your model system.
Explore the full range of lysosomal research tools and open a discussion with our specialists today.
Agnès Marcilly, MSc
Marketing Team at Tebubio
"At Tebubio, we recognise the central role of lysosomes in health and disease, and the complexities involved in studying their dynamic functions. That’s why we’ve developed a comprehensive portfolio—combining cutting-edge probes, robust assays, and expert support—to help you decode lysosomal biology with precision and ease."
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References
Source 1: Lee JH, Yang DS, Goulbourne CN, et al. “Faulty autolysosome acidification in Alzheimer's disease mouse models induces autophagic build-up of Aβ in neurons, yielding senile plaques." Nat Neurosci. 2022;25(6):688-701. doi:10.1038/s41593-022-01084-8.
Source 2: Rodriguez R, Cañeque T, Baron L, et al. “Activation of lysosomal iron triggers ferroptosis in cancer.” Preprint. Res Sq. 2024;rs.3.rs-4165774. Published 2024 Apr 8. doi:10.21203/rs.3.rs-4165774/v1.
Source 3:Machado ER, Annunziata I, van de Vlekkert D, Grosveld GC, d'Azzo A. “Lysosomes and Cancer Progression: A Malignant Liaison.” Front Cell Dev Biol. 2021;9:642494. Published 2021 Feb 26. doi:10.3389/fcell.2021.642494.
Figure 1: Desnick, Robert J, and Edward H Schuchman. "Enzyme replacement and enhancement therapies: lessons from lysosomal disorders." Nature reviews. Genetics vol. 3,12 (2002): 954-66. doi:10.1038/nrg963.
Figures 2 & 3: Courtesy of Dojindo, your trusted supplier for lysosome analyse probes.
Figure 4: Ballabio A, Bonifacino JS. “Lysosomes as dynamic regulators of cell and organismal homeostasis.” Nat Rev Mol Cell Biol. 2020;21(2):101-118. doi:10.1038/s41580-019-0185-4.
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