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Journal of Korean Neurosurgical Society > Volume 61(5); 2018 > Article
Byun, Gwak, Kwon, Kim, Shin, Lee, and Yoo: A Novel Implantable Cerebrospinal Fluid Reservoir : A Pilot Study

Abstract

Objective

The purpose of this pilot study was to examine the safety and function of the newly developed cerebrospinal fluid (CSF) reservoir called the V-Port.

Methods

The newly developed V-Port consists of a non-collapsible reservoir outlined with a titanium cage and a connector for the ventricular catheter to be assembled. It is designed to be better palpated and more durable to multiple punctures than the Ommaya reservoir. A total of nine patients diagnosed with leptomeningeal carcinomatosis were selected for V-Port insertion. Each patient was followed up for evaluation for a month after the operation.

Results

The average operation time for V-Port insertion was 42 minutes and the average incision size was 6.6 cm. The surgical technique of V-Port insertion was found to be intuitive by all neurosurgeons who participated in the pilot study. There was no obstruction or leakage of the V-Port during intrathecal chemotherapy or CSF drainage. Also, there were no complications including post-operative intracerebral hemorrhage, infection and skin problems related to the V-Port.

Conclusion

V-Port is a safe and an easy to use implantable CSF reservoir that addresses problems of other implantable CSF reservoirs. Further multicenter clinical trial is needed to prove the safety and the function of the V-Port.

INTRODUCTION

The leptomeningeal dissemination of metastatic tumors, also known as leptomeningeal carcinomatosis (LMC) is a devastating complication of both solid and hematological tumors. LMC is clinically detected in 4-7% of all cancer patients and in 5-15% of patients with leukemia and lymphoma [6]. It is becoming increasingly common in cancer patients due to enhanced detection through routine use of magnetic resonance imaging and to longer survival of these patients with better systemic control [3]. LMC can cause cranial nerve dysfunction, meningeal irritation, and increased intracranial pressure (ICP) [5], and it is associated with poor prognosis, with average survival of 2 to 4 months despite treatment [7]. The mainstay treatment for patients with LMC is intrathecal (IT) chemotherapy; the IT injection of cytotoxic drugs circumvents the blood brain barrier and blood- cerebrospinal fluid (CSF) barriers [4].
The Ommaya reservoir is a frequently used implantable CSF reservoir that helps to facilitate regular IT drug administration. It can also be used for diagnostic CSF aspiration or therapeutic CSF drainage to control increased ICP. However, there are occasional problems with the Ommaya reservoir. It may not be easily palpated in some patients due to the relatively low height of the collapsible chamber, and this is especially challenging in patients with thick scalp or those with subcutaneous hematoma formation around the reservoir. This may lead to inaccurate administration of cytotoxic drugs, which can cause complications such as skin necrosis. Furthermore, multiple compression of the collapsible chamber to determine and ensure its location may cause traction on the choroid plexus. The dome-shaped silicone port of the Ommaya reservoir is relatively fragile, and therefore, only finegauged straight needles can be used to puncture the port; larger-bored needles or multiple punctures can damage the port, ultimately leading to CSF or drug leakage. In addition, continuous CSF drainage for controlling increased ICP is difficult in patients with Ommaya reservoir because the punctured needle cannot be fixed tightly in the port.
Despite these problems with the Ommaya reservoir, there have been no notable modifications of the IT chemotherapy system to date. In this technical note, we describe a newly developed implantable CSF reservoir that addresses the problems seen with other CSF reservoirs.

MATERIALS AND METHODS

In a previously reported study from our institution, the Korean National Cancer Center [2], we introduced the novel surgical technique of installing a Chemoport as a replacement for the Ommaya reservoir in patients diagnosed with LMC. The hard outline of the port’s titanium cage made it easier to palpate than the Ommaya reservoir; in addition, the Chemoport was more durable against multiple punctures and larger-bored needles. We were also able to drain the CSF continuously in patients with increased ICP using a hooked Huber needle that was secured in the Chemoport using only closed dressings. However, the height of a Chemoport (small Celcite®; B. Braun, Boulogne Cedex, France) is nearly twice of that of a flat-bottomed Ommaya reservoir (Baxter, Heyer-Schulte, Deerfield, IL, USA). Therefore, the additional procedure of skull engraving was necessary when we installed the Chemoport. This extra step involved engraving a station approximately 4-5 mm in depth in the shape of a Chemoport using a high-speed drill; this was to secure the Chemoport on the skull and reduce the elevation of the Chemoport above the skull to prevent postoperative skin problems. Although the average operation time for Chemoport installation (54 minutes) was within an hour, it was longer by an average of 16 minutes than Ommaya reservoir insertion (38 minutes) largely due to this extra step; moreover, in order to acquire the extra space for skull engraving, we had to make larger skin incisions. In order to avoid the additional bone work and shorten the operation time, we developed a new implantable reservoir called the V-Port.

Device design

The V-Port consists of a non-collapsible port and a titanium connector where the ventricular catheter is assembled to the port (Fig. 1). The total width of the V-Port is 19 mm, and the total height is 15 mm. The non-collapsible port is made of polysulfone and epoxy instead of silicone to make it more durable against multiple punctures and larger-bored needles than the Ommaya reservoir. The diameter of the port is 1.25 mm, and it has a capacity of 0.01 mL. The port is outlined with a titanium cage in the same way as a Chemoport to make it more palpable. The outer leaf let of the titanium cage has three small holes to be used to secure the V-Port on the skull using mini-screws (3 mm). The height of the port segment of V-Port is 6 mm, which is significantly shorter than the height of the Chemoport (9.7 mm). The height was reduced to avoid the extra step of engraving a station during V-Port insertion. The V-Port prototypes were manufactured by INSUNG Medical Co., Ltd. (Wonju, Korea) and were approved by the Korean Ministry of Food and Drug Safety (approval number : 16-62) for clinical usage.

Patients

We selected nine LMC patients who were planned for IT chemotherapy for V-Port insertion. All patients had to be over 19 years of age and had to score over 60 on the Karnofsky performance scale. The demographic characteristics of these patients are presented in Table 1. We confirmed the diagnosis of LMC by the presence of malignant cells in the CSF. Patients and guardians provided written consent for V-Port insertion after the attending physician thoroughly explained the possible risks of the procedure. This pilot study for V-Port insertion was approved by the institutional review board of the National Cancer Center Korea (IRB approval number : IRB NCC2016-0244).

Surgical technique

The V-Ports were inserted by four experienced neurosurgeons at the Korean National Cancer Center. The V-Port insertion is similar to the well-established method of stereotactic insertion of the Ommaya reservoir [1]. The patient was put in a supine position with the head resting on a horseshoe Mayfeld head holder. Aseptic dressing was applied after the frameless stereotactic system (AxiEM™ SYSTEM, Medtronic, Minneapolis, MN, USA) was set up. A semicircular incision was made around the right Kocher’s point and a small burr hole (8-10 mm in diameter) was made. A ventricular catheter was inserted into the right frontal horn via the planned trajectory to the appropriate depth using the stereotactic system. A ventricular catheter from the Ommaya reservoir set was used. After the ventricular access was confirmed by visualizing CSF flow through the catheter, the catheter was cut to the appropriate length. The catheter was connected to the titanium connector portion of the V-Port and tied with a black silk suture to secure it. The outer titanium leaflet of the V-Port was then placed on the outer layer of the skull and secured using three 3-mm mini-screws (Fig. 2). The V-Port was punctured with a small needle for a final check of its function, and the wound was closed layer by layer.

RESULTS

The total operation time, incision size, and estimated blood loss were recorded during each operation. Each neurosurgeon provided feedback about his experiences and impressions of the V-Port. Immediate postoperative CT scans were taken to check for intracerebral hemorrhage (ICH) and malposition of the catheter; the patients were then transferred to their respective oncologists for IT chemotherapy. Each patient was followed up for four weeks after the operation and evaluated for signs of postoperative infection and skin problems. The function and palpability of the V-Port were evaluated during IT chemotherapy and/or CSF drainage.
The average operation time for V-Port insertion was 42 minutes, with an average incision size of 6.6 cm and an estimated blood loss of 16.6 mL. All four neurosurgeons who performed the operation found the surgical technique of V-Port insertion to be intuitive because it was similar to inserting a burr-hole-type Ommaya reservoir. The surgeons also subjectively found V-Port insertion to be much easier than Chemoport installation because it required smaller skin incisions and less bone work.
The average follow-up duration was 26 days because two patients died before the 4-week mark. Ultimately only four patients underwent IT chemotherapy; the oncologists decided on chemotherapy based on the patient’s functional status, the rate of disease progression, and the patient’s and/or guardian’s preference. Seven patients underwent CSF drainage at least once for ICP control, and of those seven, two underwent continuous CSF drainage because the ICP was not effectively controlled by intermittent drainage. A hooked Huber needle was secured in the V-Port and connected to an extra-ventricular drainage bag for continuous drainage of the CSF (Fig. 3). The large-bored Huber needle was well tolerated by the V-Port and was secured well in the V-Port using only closed dressings. The V-Port was easily palpated in all cases, even in patients with relatively thick scalp. There was no obstruction or leakage of the V-Port during IT chemotherapy or CSF drainage. Furthermore, there were no complications including postoperative ICH, infection, and skin problems related to the V-Port.

DISCUSSION

In this pilot study, we describe a newly developed implantable CSF reservoir called the V-Port and the surgical technique for its insertion. Until now, our institution has actively adopted the use of Chemoports rather than Ommaya reservoirs in LMC patients because they are easier to palpate and more durable against larger-bored needles than the Ommaya reservoir; in addition, we were able to continuously drain the CSF in patients with uncontrolled increased ICP using the Chemoport. However, due to the height of the Chemoport, we had to engrave a station for it on the skull, which led to longer operation times and larger incisions.
We addressed these problems by making the port of the V-Port much shorter than the Chemoport’s while maintaining the titanium cage around the port. The average operation time was shorter than that for Chemoport insertion, and the surgical technique for its insertion was easy and intuitive for the neurosurgeons. Furthermore, there were no malfunctions or complications related to the V-Port during our pilot study.
We believe that the V-Port is a safe and an easy-to-use device that could substitute for previous implantable CSF reservoirs. We acknowledge that a larger clinical trial is necessary before the V-Port can be widely accepted. Therefore, we are currently conducting a nationwide multicenter clinical trial based on this pilot study to further test the V-Port’s safety and function.

CONCLUSION

V-Port is a safe and an easy to use implantable CSF reservoir that addresses problems of other implantable CSF reservoirs. Further multicenter clinical trial is needed to prove the safety and the function of the V-Port.

Notes

No potential conflict of interest relevant to this article was reported.

INFORMED CONSENT

Informed consent was obtained from all individual participants included in this study.

Acknowledgements

This research was supported by the Ministry of Trade, Industry & Energy (MOTIE), Korea Institute for Advancement of Technology (KIAT) through the Encouragement Program for The Industries of Economic Cooperation Region (R0003970, 2015).
This research was supported by the Ministry of Trade, Industry & Energy (MOTIE), Korea Institute for Advancement of Technology (KIAT) through the Encouragement Program for The Industries of Economic Cooperation Region (10062968, Development of chemoport for measurement of the brain pressure).

Fig. 1.
Photographs of the V-Port. The V-Port is constituted of (A) a noncollapsible reservoir outlined with a titanium cage and (B) a connector for the ventricular catheter to be assembled. (C) The three holes of the titanium outer leaflet are designed to secure the V-Port on the skull using mini screws.
jkns-2018-0098f1.jpg
Fig. 2.
Intraoperative photograph depicting V-Port insertion.
jkns-2018-0098f2.jpg
Fig. 3.
Photographs of CSF being continuously drained. A : A hooked Huber needle was secured in the V-Port. B : The Huber needle was connected to an extra-ventricular drainage bag for continuous drainage of the CSF. CSF : cerebrospinal fluid.
jkns-2018-0098f3.jpg
Table 1.
Demographic, operative, and treatment data for nine patients who underwent V-Port insertion
Case No. Sex Age Primary cancer (subtype) Operation
Treatment
FU (days) Complications
Operation time (minutes) Incision size (cm) EBL (mL) Intrathecal chemotherapy CSF drainage for ICP control
Intermittent Continuos
1 F 46 NSCLC (ADC) 35 7.5 20 + + + 28 None
2 F 47 NSCLC (ADC) 57 7.5 20 - + - 18 None
3 F 56 Breast (IDC) 47 6.5 20 + + - 28 None
4 M 71 Unknown 32 6.5 20 + - - 28 None
5 F 61 SCLC 31 7 10 + - - 28 None
6 M 54 NSCLC (ADC) 40 5.5 10 - + - 28 None
7 M 65 NSCLC (ADC) 49 7 20 - + - 28 None
8 M 51 NSCLC (LCNEC) 38 5.5 10 - + + 21 None
9 F 71 NSCLC (ADC) 50 6.5 20 - + - 28 None

EBL : estimated blood loss, CSF : cerebrospinal fluid, ICP : intracranial pressure, FU : follow-up, NSCLC : non-small cell lung cancer, ADC : adenocarcinoma, IDC : invasive ductal carcinoma, LCNEC : large cell neuroendocrine carcinoma

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