Scientists have long sought to understand how vascular networks supply blood
and oxygen to cells throughout the body. Recent work focuses on principles that
constrain how vessel size changes through branching generations from the aorta
to capillaries and uses scaling exponents to quantify these changes. Prominent
scaling theories predict that combinations of these exponents explain how
metabolic, growth, and other biological rates vary with body size.
Nevertheless, direct measurements of individual vessel segments have been
limited because existing techniques for measuring vasculature are invasive,
time consuming, and technically difficult. We developed software that extracts
the length, radius, and connectivity of in vivo vessels from contrast-enhanced
3D Magnetic Resonance Angiography. Using data from 20 human subjects, we
calculated scaling exponents by four methods--two derived from local properties
of branching junctions and two from whole-network properties. Although these
methods are often used interchangeably in the literature, we do not find
general agreement between these methods, particularly for vessel lengths.
Measurements for length of vessels also diverge from theoretical values, but
those for radius show stronger agreement. Our results demonstrate that vascular
network models cannot ignore certain complexities of real vascular systems and
indicate the need to discover new principles regarding vessel lengths