Diffuse correlation spectroscopy measurements of blood flow using 1064 nm light

Stefan Carp; Davide Tamborini; Dibbyan Mazumder; Kuan-Cheng Wu; Mitchell Robinson; Kimberly Stephens; Oleg Shatrovoy; Niyom Lue; Nisan Ozana; Megan Blackwell; Maria Angela Franceschini

doi:10.1117/1.JBO.25.9.097003

Diffuse correlation spectroscopy measurements of blood flow using 1064 nm light

J Biomed Opt. 2020 Sep;25(9):097003. doi: 10.1117/1.JBO.25.9.097003.

Authors

Stefan Carp^{1

2}, Davide Tamborini^{1

2}, Dibbyan Mazumder^{1

2}, Kuan-Cheng Wu^{1

2

3}, Mitchell Robinson^{1

2

4}, Kimberly Stephens^{1

2}, Oleg Shatrovoy⁵, Niyom Lue⁴, Nisan Ozana^{1

2}, Megan Blackwell⁵, Maria Angela Franceschini^{1

2}

Affiliations

¹ Athinoula A. Martinos Ctr. for Biomedical Imaging, Massachusetts General Hospital, United States.
² Harvard Medical School, United States.
³ Boston Univ., United States.
⁴ Massachusetts Institute of Technology, United States.
⁵ MIT Lincoln Lab., United States.

Abstract

Significance: Diffuse correlation spectroscopy (DCS) is an established optical modality that enables noninvasive measurements of blood flow in deep tissue by quantifying the temporal light intensity fluctuations generated by dynamic scattering of moving red blood cells. Compared with near-infrared spectroscopy, DCS is hampered by a limited signal-to-noise ratio (SNR) due to the need to use small detection apertures to preserve speckle contrast. However, DCS is a dynamic light scattering technique and does not rely on hemoglobin contrast; thus, there are significant SNR advantages to using longer wavelengths (>1000 nm) for the DCS measurement due to a variety of biophysical and regulatory factors.

Aim: We offer a quantitative assessment of the benefits and challenges of operating DCS at 1064 nm versus the typical 765 to 850 nm wavelength through simulations and experimental demonstrations.

Approach: We evaluate the photon budget, depth sensitivity, and SNR for detecting blood flow changes using numerical simulations. We discuss continuous wave (CW) and time-domain (TD) DCS hardware considerations for 1064 nm operation. We report proof-of-concept measurements in tissue-like phantoms and healthy adult volunteers.

Results: DCS at 1064 nm offers higher intrinsic sensitivity to deep tissue compared with DCS measurements at the typically used wavelength range (765 to 850 nm) due to increased photon counts and a slower autocorrelation decay. These advantages are explored using simulations and are demonstrated using phantom and in vivo measurements. We show the first high-speed (cardiac pulsation-resolved), high-SNR measurements at large source-detector separation (3 cm) for CW-DCS and late temporal gates (1 ns) for TD-DCS.

Conclusions: DCS at 1064 nm offers a leap forward in the ability to monitor deep tissue blood flow and could be especially useful in increasing the reliability of cerebral blood flow monitoring in adults.

Keywords: Monte Carlo simulations; blood flow; diffuse correlation spectroscopy; near-infrared; short-wave infrared.

Publication types

Research Support, N.I.H., Extramural
Research Support, U.S. Gov't, Non-P.H.S.

MeSH terms

Hemodynamics*
Humans
Regional Blood Flow
Reproducibility of Results
Signal-To-Noise Ratio
Spectroscopy, Near-Infrared*

Abstract

Publication types

MeSH terms

Grants and funding