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Echogenic Polymer Coating

Does It Improve Needle Visualization in Sonographically Guided Biopsy?

¹ All authors: Department of Radiology, Duke University Medical Center, Box 3808, Durham, NC 27710.

Received August 17, 2001; accepted after revision October 30, 2001.

 
Address correspondence to E. K. Paulson.

Introduction

Top Introduction Subjects and Methods Results Discussion References

 
Percutaneous biopsy and aspiration in the abdomen and pelvis are increasingly performed with sonographic guidance, which is safe and cost-effective [1, 2]. However, one of the limitations of sonographic guidance has been difficulty in visualizing the needle [3,4,5,6].

A thin, biocompatible polymer coating has been produced that can be applied to metallic surfaces [7]. This polymer coating is applied by the manufacturer (STS Biopolymers, Henrietta, NY) by a process of dipping followed by exposure to water and air drying at slightly elevated temperatures. The polymer film has a porous microstructure that entraps microbubbles of air. As the coated needle is advanced into tissue, air bubbles trapped in the polymeric coating create multiple specular reflectors on the surface of the needle. This polymer coating has been shown to enhance needle visualization in an animal study [7]. The purpose of our study was to test this polymer-coated needle in clinical practice.

Subjects and Methods

Top Introduction Subjects and Methods Results Discussion References

 
This was a prospective, randomized study with institutional review board approval. We had no specific funding for the project. Patients scheduled for sonographically guided biopsies in which a 20-gauge aspirating needle was to be used were considered suitable for enrollment. After we obtained their written informed consent, patients were chosen at random to have an initial biopsy performed with either a polymer-coated 20-gauge Franseen needle or a standard 20-gauge Franseen needle (Allegiance Healthcare, McGaw Park, IL). If more than one needle pass was required, alternate needles were used.

We enrolled 27 patients between October 1, 2000 and February 28, 2001. Our study group consisted of 12 men and 15 women who ranged in age from 31 to 86 years (mean age, 56 years). The patients underwent the following biopsies: liver (n = 15), lymph node (n = 3), pelvis (n = 2), pancreas (n = 2), adrenal gland (n = 2), thyroid (n = 1), spleen (n = 1), and abdominal wall (n = 1). Of the 27 patients, four underwent a single needle pass, and the remainder underwent more than one needle pass.

A 20-gauge needle was used in all biopsies, but the operators were unaware of whether the needle was coated or uncoated. All biopsies were performed using a sonographic unit (700 Logiq; General Electric Medical Systems, Milwaukee, WI) with either a 3.5-MHz curved electronic phased array transducer or a 7- to 10-MHz linear array transducer, depending on the target organ. The appropriate needle guide for the transducer was used at each needle pass to ensure that the angle of the needle relative to the transducer was identical for biopsies with coated and uncoated needles. A cytopathologist was present at each biopsy who determined when sufficient tissue had been obtained for diagnostic purposes. Once the diagnostic material was obtained, no additional needle passes were performed.

At the end of each biopsy procedure, the operator completed a questionnaire indicating the transducer used, the target organ biopsied, and the lesion depth and size. The operator graded visibility of the needle tip and shaft at each needle pass as follows: grade 1, not visualized at all or poorly visualized, with the needle tip and shaft being isoechoic or only slightly more echogenic than the background parenchyma; grade 2, the tip or shaft was visualized with some difficulty, with the shaft and tip readily identified as being more echogenic than the background parenchyma but not seen in their entirety; grade 3, excellent visibility, with shaft and tip strongly echogenic relative to their background and visualized in their entirety.

The grade of visibility of the needle shaft and tip was assessed by the Wilcoxon-Mann-Whitney test. The Kendall's tau b correlation coefficient was determined for lesion depth and the grade of visualization of both the needle tip and the needle shaft.

Results

Top Introduction Subjects and Methods Results Discussion References

 
Fifty-four needle passes were made in 27 patients. Twenty-nine passes were made with polymer-coated needles (Fig. 1), and 25 passes were made with uncoated needles. The target lesions biopsied ranged from 2 to 14 cm deep to the skin surface (mean depth, 7 cm).

View larger version (59K): [in this window] [in a new window] [as a PowerPoint slide]   Fig. 1. —Photograph of polymer-coated 20-gauge Franseen needle (Allegiance Healthcare, McGaw Park, IL) with magnified image of needle tip (inset). Magnified view shows needle tip and distal edge of polymer coating (arrow). Polymer coating is barely discernible.

The operator visualized the needle tip (rated as grade 2 or grade 3 visualization) in 100% of passes with polymer-coated needles and 84% of passes with uncoated needles. The tip of the coated needle was clearly visualized (grade 3) by the operator in 66% of passes compared with only 32% of passes with the uncoated needle (p < 0.0009) (Fig. 2A,2B). The needle shaft was visualized (grade 2 or grade 3) by the operator in 79% of passes with the coated needle and 28% of passes with the uncoated needle. The shaft of the coated needle was visualized clearly throughout its length by the operator in 27% of passes compared with only 4% of passes made with the uncoated needle (p < 0.0001). We found no correlation between depth of lesion and operator visibility of the needle shaft (Kendall's tau b coefficient = 0.023, p = 0.83) or needle tip (Kendall's tau b coefficient = -0.05, p = 0.63).

View larger version (128K): [in this window] [in a new window] [as a PowerPoint slide]   Fig. 2A. —Sonographically guided biopsy of porta hepatis lymph node via lateral segment of liver in 39-year-old man with hepatitis B. Sonogram of biopsy using polymer-coated 20-gauge Franseen needle (Allegiance Healthcare, McGaw Park, IL) shows clear visualization of needle tip (straight arrow) and shaft (curved arrow).

View larger version (123K): [in this window] [in a new window] [as a PowerPoint slide]   Fig. 2B. —Sonographically guided biopsy of porta hepatis lymph node via lateral segment of liver in 39-year-old man with hepatitis B. Sonogram of biopsy using uncoated 20-gauge Franseen needle shows partial visualization of needle shaft (curved arrow) and suboptimal visualization of needle tip (straight arrow).

Discussion

Top Introduction Subjects and Methods Results Discussion References

 
Sonography is portable; it does not use ionizing radiation; and it can provide guidance in multiple planes. Although sonography is increasingly used to guide needle placement in interventional procedures, difficulty in obtaining adequate visualization of the needle continues to be a significant limitation [3,4,5,6].

STS Biopolymers has produced a polymer coating, approved by the United States Food and Drug Administration, that can be applied to the surface of needles and other devices such as catheters. In this study, we found that the polymer-coated needle shaft and tip were better visualized by the operator than those of the standard needle (p < 0.0001 and p < 0.0009, respectively), independent of lesion depth.

Although many radiologists performing biopsies with sonographic guidance may have a preference for the freehand technique, our study found that using the needle guide created comparable angles between the needle and the transducer for biopsies with coated and uncoated needles [8].

It has been reported that polymer-coated needles may lose echogenicity when used for several passes, likely as a result of microbubbles of air being replaced by fluid [7]. The results of our study cannot be used to corroborate this observation because, in our practice, we routinely use a new needle for each pass. However, we did encounter a number of instances in which visualization of the shaft and tip of the polymer-coated needle was suboptimal. The shaft of the coated needle was poorly visualized or not visualized by the operator in 21% of cases, and it was seen with some difficulty (grade 2) in 52% of passes. Visualization of the shaft of both polymer-coated and uncoated needles was more difficult when the background parenchyma was echogenic, particularly in areas with an abundance of fatty tissue, such as in the retroperitoneum or in a fatty liver.

Although our study is limited to evaluation of only the 20-gauge polymer-coated needle, it can be suggested that polymer coating is likely to enhance visualization of larger bore needles as well. Larger bore needles are generally better visualized on sonography than smaller needles, and previous investigators reported improved visualization of 22-gauge needles with polymer coating [7].

In conclusion, we believe polymer coating of needles is a promising innovation that improves both needle shaft and tip visibility in clinical practice compared with a standard uncoated needle. Unlike many innovations, the polymer-coated needle does not require the development of a new skill by the radiologist or the acquisition of additional equipment [3,4,5,6]. The availability of these needles may further encourage the transition from CT guidance to sonographic guidance for percutaneous intervention. Further research and development are required to ensure a more consistent performance and consistent visibility for the interventional radiologist using this polymer coating for sonographically guided biopsies.

References

Top Introduction Subjects and Methods Results Discussion References

 

1. Kliewer MA, Sheafor DH, Paulson EK, Helsper RS, Hertzberg BS, Nelson RC. Percutaneous liver biopsy: a cost—benefit analysis comparing sonographic and CT guidance. AJR 1999;173:1199 -1202[Abstract/Free Full Text]
2. Memel DS, Dodd GD III, Escola CC. Efficacy of sonography as a guidance technique for biopsy of abdominal, pelvic, and retroperitoneal lymph nodes. AJR 1996;167:957 -962[Abstract/Free Full Text]
3. Feld R, Needleman L, Goldberg BB. Use of a needle-vibrating device and color Doppler imaging for sonographically guided invasive procedures. AJR 1997;168:255 -256[Free Full Text]
4. Howard MH, Nelson RC, Paulson EK, Kliewer MA, Sheafor DH. An electronic device for needle placement during sonographically guided percutaneous intervention. Radiology 2001;218:905 -911[Abstract/Free Full Text]
5. Winsberg F, Mitty MA, Shapiro RS, Yeh MC. Use of an acoustic transponder for US visualization of biopsy needles. Radiology 1991;180:877 -878[Abstract/Free Full Text]
6. Perrella RR, Kimrre-Smith C, Tessler FN, Ragavendra N, Grant EG. A new electronically enhanced biopsy system: value in improving needle-tip visibility during sonographically guided interventional procedures. AJR 1992;158:195 -198[Abstract/Free Full Text]
7. Gottlieb RM, Robinette WB, Rubens DJ, Hartley DF, Fultz PJ, Violante MR. Coating agent permits improved visualization of biopsy needles during sonography. AJR 1998;171:1301 -1302[Free Full Text]
8. Caturelli E, Giacobbe A, Facciorusso D, et al. Free-hand technique with ordinary antisepsis in abdominal US-guided fine-needle punctures: three-year experience. Radiology 1996;199:721 -723[Abstract/Free Full Text]

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