Caspases are proteases that carry out apoptosis; they are made as inactive forms and, once activated, cut specific cellular proteins to dismantle the cell in a controlled way.

Why is apoptosis important during development?

Programmed death removes cells that are no longer needed, helping to sculpt structures such as digits and to eliminate excess cells, which is essential for normal development.

Apoptosis and Programmed Cell Death

Apoptosis is an orderly, genetically controlled form of cell death that dismantles a cell cleanly, a process essential for shaping tissues and removing unwanted cells.

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Definition

Apoptosis is a regulated form of programmed cell death in which a cell activates an internal proteolytic program that dismantles it into membrane-bound fragments for clean removal.

Scope

This topic covers the morphology and purpose of apoptosis, the caspase proteases that execute it, the intrinsic mitochondrial and extrinsic death-receptor pathways that activate them, the regulatory Bcl-2 protein family, and the clearance of apoptotic cells.

Core questions

What distinguishes apoptosis from accidental cell death?
What roles do caspases play in executing apoptosis?
How do the intrinsic and extrinsic pathways trigger apoptosis?
How is the decision to live or die regulated by the Bcl-2 family?

Key theories

Apoptosis as a regulated program: Kerr, Wyllie, and Currie identified apoptosis as a distinct, controlled mode of cell death with characteristic morphology, separate from passive necrosis.
Genetic control of programmed cell death: Genetic analysis in the nematode revealed defined genes that direct programmed cell death, establishing a conserved molecular machinery underlying apoptosis.

Mechanisms

Apoptosis is executed by caspases, proteases that exist as inactive precursors and, once activated, cleave many cellular targets to dismantle the cell while preserving membrane integrity. The intrinsic pathway responds to internal stress by permeabilizing mitochondria to release factors that activate caspases, governed by the balance of pro- and anti-apoptotic Bcl-2 family proteins. The extrinsic pathway is triggered by death-receptor ligands at the cell surface. The resulting apoptotic bodies are recognized and engulfed by neighboring cells, avoiding inflammation.

Clinical relevance

Apoptosis sculpts developing tissues, removes excess or damaged cells, and balances cell production, making it foundational to development and homeostasis. The treatment here is descriptive and non-prescriptive.

History

The 1972 description of apoptosis by Kerr, Wyllie, and Currie defined it morphologically; Horvitz, working in the nematode model established by Brenner, identified the genes that control programmed death and revealed their conservation.

Key figures

John Kerr
Andrew Wyllie
Robert Horvitz
Sydney Brenner

Seminal works

kerr1972
horvitz1986

Frequently asked questions

What are caspases?: Caspases are proteases that carry out apoptosis; they are made as inactive forms and, once activated, cut specific cellular proteins to dismantle the cell in a controlled way.
Why is apoptosis important during development?: Programmed death removes cells that are no longer needed, helping to sculpt structures such as digits and to eliminate excess cells, which is essential for normal development.